thesis.lyx 420 KB

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  225. \begin_layout Title
  226. Bioinformatic analysis of complex, high-throughput genomic and epigenomic
  227. data in the context of immunology and transplant rejection
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  229. \begin_layout Author
  230. A thesis presented
  231. \begin_inset Newline newline
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  233. by
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  236. Ryan C.
  237. Thompson
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  240. to
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  243. The Scripps Research Institute Graduate Program
  244. \begin_inset Newline newline
  245. \end_inset
  246. in partial fulfillment of the requirements for the degree of
  247. \begin_inset Newline newline
  248. \end_inset
  249. Doctor of Philosophy in the subject of Biology
  250. \begin_inset Newline newline
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  252. for
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  255. The Scripps Research Institute
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  258. La Jolla, California
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  260. \begin_layout Date
  261. October 2019
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  267. To remove TODOs and watermark: Add
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  273. to the document class custom options.
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  287. [Copyright notice]
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  294. addcontentsline{toc}{chapter}{Thesis acceptance form}
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  299. [Thesis acceptance form]
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  346. \end_layout
  347. \begin_layout Enumerate
  348. Wrap every occurrence of the term in Insert -> Custom Insets -> Glossary
  349. Term (use appropriate variants for caiptal, plural, etc.), using Edit ->
  350. Find & Replace (Advanced).
  351. Skip section headers and float captions.
  352. \end_layout
  353. \begin_layout Plain Layout
  354. \begin_inset CommandInset href
  355. LatexCommand href
  356. target "https://ctan.org/pkg/glossaries?lang=en"
  357. literal "false"
  358. \end_inset
  359. \begin_inset CommandInset href
  360. LatexCommand href
  361. target "https://ctan.org/pkg/glossaries-extra"
  362. literal "false"
  363. \end_inset
  364. \end_layout
  365. \end_inset
  366. \end_layout
  367. \begin_layout Standard
  368. \align center
  369. \begin_inset ERT
  370. status open
  371. \begin_layout Plain Layout
  372. \backslash
  373. renewcommand*{
  374. \backslash
  375. glossaryname}{List of Abbreviations}%
  376. \end_layout
  377. \begin_layout Plain Layout
  378. \backslash
  379. printglossaries
  380. \end_layout
  381. \end_inset
  382. \end_layout
  383. \begin_layout List of TODOs
  384. \end_layout
  385. \begin_layout Chapter*
  386. Abstract
  387. \end_layout
  388. \begin_layout Standard
  389. \begin_inset Note Note
  390. status open
  391. \begin_layout Plain Layout
  392. It is included as an integral part of the thesis and should immediately
  393. precede the introduction.
  394. \end_layout
  395. \begin_layout Plain Layout
  396. Preparing your Abstract.
  397. Your abstract (a succinct description of your work) is limited to 350 words.
  398. UMI will shorten it if they must; please do not exceed the limit.
  399. \end_layout
  400. \begin_layout Itemize
  401. Include pertinent place names, names of persons (in full), and other proper
  402. nouns.
  403. These are useful in automated retrieval.
  404. \end_layout
  405. \begin_layout Itemize
  406. Display symbols, as well as foreign words and phrases, clearly and accurately.
  407. Include transliterations for characters other than Roman and Greek letters
  408. and Arabic numerals.
  409. Include accents and diacritical marks.
  410. \end_layout
  411. \begin_layout Itemize
  412. Do not include graphs, charts, tables, or illustrations in your abstract.
  413. \end_layout
  414. \end_inset
  415. \end_layout
  416. \begin_layout Standard
  417. \begin_inset Flex TODO Note (inline)
  418. status open
  419. \begin_layout Plain Layout
  420. Obviously the abstract gets written last.
  421. \end_layout
  422. \end_inset
  423. \end_layout
  424. \begin_layout Chapter*
  425. Notes to draft readers
  426. \end_layout
  427. \begin_layout Standard
  428. Thank you so much for agreeing to read my thesis and give me feedback on
  429. it.
  430. What you are currently reading is a rough draft, in need of many revisions.
  431. You can always find the latest version at
  432. \begin_inset CommandInset href
  433. LatexCommand href
  434. target "https://mneme.dedyn.io/~ryan/Thesis/thesis.pdf"
  435. literal "false"
  436. \end_inset
  437. .
  438. the PDF at this link is updated periodically with my latest revisions,
  439. but you can just download the current version and give me feedback on that.
  440. Don't worry about keeping up with the updates.
  441. \end_layout
  442. \begin_layout Standard
  443. As for what feedback I'm looking for, first of all, don't waste your time
  444. marking spelling mistakes and such.
  445. I haven't run a spell checker on it yet, so let me worry about that.
  446. Also, I'm aware that many abbreviations are not properly introduced the
  447. first time they are used, so don't worry about that either.
  448. However, if you see any glaring formatting issues, such as a figure being
  449. too large and getting cut off at the edge of the page, please note them.
  450. In addition, if any of the text in the figures is too small, please note
  451. that as well.
  452. \end_layout
  453. \begin_layout Standard
  454. Beyond that, what I'm mainly interested in is feedback on the content.
  455. For example: does the introduction flow logically, and does it provide
  456. enough background to understand the other chapters? Does each chapter make
  457. it clear what work and analyses I have done? Do the figures clearly communicate
  458. the results I'm trying to show? Do you feel that the claims in the results
  459. and discussion sections are well-supported? There's no need to suggest
  460. improvements; just note areas that you feel need improvement.
  461. Additionally, if you notice any un-cited claims in any chapter, please
  462. flag them for my attention.
  463. Similarly, if you discover any factual errors, please note them as well.
  464. \end_layout
  465. \begin_layout Standard
  466. You can provide your feedback in whatever way is most convenient to you.
  467. You could mark up this PDF with highlights and notes, then send it back
  468. to me.
  469. Or you could collect your comments in a separate text file and send that
  470. to me, or whatever else you like.
  471. However, if you send me your feedback in a separate document, please note
  472. a section/figure/table number for each comment, and
  473. \emph on
  474. also
  475. \emph default
  476. send me the exact PDF that you read so I can reference it while reading
  477. your comments, since as mentioned above, the current version I'm working
  478. on will have changed by that point (which might include shuffling sections
  479. and figures around, changing their numbers).
  480. One last thing: you'll see a bunch of text in orange boxes throughout the
  481. PDF.
  482. These are notes to myself about things that need to be fixed later, so
  483. if you see a problem noted in an orange box, that means I'm already aware
  484. of it, and there's no need to comment on it.
  485. \end_layout
  486. \begin_layout Standard
  487. My thesis is due Thursday, October 10th, so in order to be useful to me,
  488. I'll need your feedback at least several days before that, ideally by Monday,
  489. October 7th.
  490. If you have limited time and are unable to get through the whole thesis,
  491. please focus your efforts on Chapters 1 and 2, since those are the roughest
  492. and most in need of revision.
  493. Chapter 3 is fairly short and straightforward, and Chapter 4 is an adaptation
  494. of a paper that's already been through a few rounds of revision, so they
  495. should be a lot tighter.
  496. If you can't spare any time between now and then, or if something unexpected
  497. comes up, I understand.
  498. Just let me know.
  499. \end_layout
  500. \begin_layout Standard
  501. Thanks again for your help, and happy reading!
  502. \end_layout
  503. \begin_layout Chapter
  504. Introduction
  505. \end_layout
  506. \begin_layout Standard
  507. \begin_inset ERT
  508. status collapsed
  509. \begin_layout Plain Layout
  510. \backslash
  511. glsresetall
  512. \end_layout
  513. \end_inset
  514. \begin_inset Note Note
  515. status collapsed
  516. \begin_layout Plain Layout
  517. Reintroduce all abbreviations
  518. \end_layout
  519. \end_inset
  520. \end_layout
  521. \begin_layout Section
  522. \begin_inset CommandInset label
  523. LatexCommand label
  524. name "sec:Biological-motivation"
  525. \end_inset
  526. Biological motivation
  527. \end_layout
  528. \begin_layout Standard
  529. \begin_inset Flex TODO Note (inline)
  530. status open
  531. \begin_layout Plain Layout
  532. Rethink the subsection organization after the intro is written.
  533. \end_layout
  534. \end_inset
  535. \end_layout
  536. \begin_layout Subsection
  537. Rejection is the major long-term threat to organ and tissue allografts
  538. \end_layout
  539. \begin_layout Standard
  540. Organ and tissue transplants are a life-saving treatment for people who
  541. have lost the function of an important organ.
  542. In some cases, it is possible to transplant a patient's own tissue from
  543. one area of their body to another, referred to as an autograft.
  544. This is common for tissues that are distributed throughout many areas of
  545. the body, such as skin and bone.
  546. However, in cases of organ failure, there is no functional self tissue
  547. remaining, and a transplant from another person – a donor – is required.
  548. This is referred to as an allograft
  549. \begin_inset CommandInset citation
  550. LatexCommand cite
  551. key "Valenzuela2017"
  552. literal "false"
  553. \end_inset
  554. .
  555. \end_layout
  556. \begin_layout Standard
  557. \begin_inset Flex TODO Note (inline)
  558. status open
  559. \begin_layout Plain Layout
  560. How much mechanistic detail is needed here? My work doesn't really go into
  561. specific rejection mechanisms, so I think it's best to keep it basic.
  562. \end_layout
  563. \end_inset
  564. \end_layout
  565. \begin_layout Standard
  566. Because an allograft comes from a donor who is genetically distinct from
  567. the recipient (with rare exceptions), genetic variants in protein-coding
  568. regions affect the polypeptide sequences encoded by the affected genes,
  569. resulting in protein products in the allograft that differ from the equivalent
  570. proteins produced by the graft recipient's own tissue.
  571. As a result, without intervention, the recipient's immune system will eventuall
  572. y identify the graft as foreign tissue and begin attacking it, eventually
  573. resulting in failure and death of the graft, a process referred to as transplan
  574. t rejection
  575. \begin_inset CommandInset citation
  576. LatexCommand cite
  577. key "Murphy2012"
  578. literal "false"
  579. \end_inset
  580. .
  581. Rejection is the most significant challenge to the long-term health and
  582. survival of an allograft
  583. \begin_inset CommandInset citation
  584. LatexCommand cite
  585. key "Valenzuela2017"
  586. literal "false"
  587. \end_inset
  588. .
  589. Like any adaptive immune response, graft rejection generally occurs via
  590. two broad mechanisms: cellular immunity, in which CD8
  591. \begin_inset Formula $^{+}$
  592. \end_inset
  593. T-cells recognizing graft-specific antigens induce apoptosis in the graft
  594. cells; and humoral immunity, in which B-cells produce antibodies that bind
  595. to graft proteins and direct an immune response against the graft
  596. \begin_inset CommandInset citation
  597. LatexCommand cite
  598. key "Murphy2012"
  599. literal "false"
  600. \end_inset
  601. .
  602. In either case, rejection shows most of the typical hallmarks of an adaptive
  603. immune response, in particular mediation by CD4
  604. \begin_inset Formula $^{+}$
  605. \end_inset
  606. T-cells and formation of immune memory.
  607. \end_layout
  608. \begin_layout Subsection
  609. Diagnosis and treatment of allograft rejection is a major challenge
  610. \end_layout
  611. \begin_layout Standard
  612. \begin_inset Flex TODO Note (inline)
  613. status open
  614. \begin_layout Plain Layout
  615. Maybe talk about HLA matching and why it's not an option most of the time.
  616. \end_layout
  617. \end_inset
  618. \end_layout
  619. \begin_layout Standard
  620. To prevent rejection, allograft recipients are treated with immune suppressive
  621. drugs
  622. \begin_inset CommandInset citation
  623. LatexCommand cite
  624. key "Kowalski2003,Murphy2012"
  625. literal "false"
  626. \end_inset
  627. .
  628. The goal is to achieve sufficient suppression of the immune system to prevent
  629. rejection of the graft without compromising the ability of the immune system
  630. to raise a normal response against infection.
  631. As such, a delicate balance must be struck: insufficient immune suppression
  632. may lead to rejection and ultimately loss of the graft; excessive suppression
  633. leaves the patient vulnerable to life-threatening opportunistic infections
  634. \begin_inset CommandInset citation
  635. LatexCommand cite
  636. key "Murphy2012"
  637. literal "false"
  638. \end_inset
  639. .
  640. Because every patient's matabolism is different, achieving this delicate
  641. balance requires drug dosage to be tailored for each patient.
  642. Furthermore, dosage must be tuned over time, as the immune system's activity
  643. varies over time and in response to external stimuli with no fixed pattern.
  644. In order to properly adjust the dosage of immune suppression drugs, it
  645. is necessary to monitor the health of the transplant and increase the dosage
  646. if evidence of rejection or alloimmune activity is observed.
  647. \end_layout
  648. \begin_layout Standard
  649. However, diagnosis of rejection is a significant challenge.
  650. Early diagnosis is essential in order to step up immune suppression before
  651. the immune system damages the graft beyond recovery
  652. \begin_inset CommandInset citation
  653. LatexCommand cite
  654. key "Israeli2007"
  655. literal "false"
  656. \end_inset
  657. .
  658. The current gold standard test for graft rejection is a tissue biopsy,
  659. examined for visible signs of rejection by a trained histologist
  660. \begin_inset CommandInset citation
  661. LatexCommand cite
  662. key "Kurian2014"
  663. literal "false"
  664. \end_inset
  665. .
  666. When a patient shows symptoms of possible rejection, a
  667. \begin_inset Quotes eld
  668. \end_inset
  669. for cause
  670. \begin_inset Quotes erd
  671. \end_inset
  672. biopsy is performed to confirm the diagnosis, and immune suppression is
  673. adjusted as necessary.
  674. However, in many cases, the early stages of rejection are asymptomatic,
  675. known as
  676. \begin_inset Quotes eld
  677. \end_inset
  678. sub-clinical
  679. \begin_inset Quotes erd
  680. \end_inset
  681. rejection.
  682. In light of this, is is now common to perform
  683. \begin_inset Quotes eld
  684. \end_inset
  685. protocol biopsies
  686. \begin_inset Quotes erd
  687. \end_inset
  688. at specific times after transplantation of a graft, even if no symptoms
  689. of rejection are apparent, in addition to
  690. \begin_inset Quotes eld
  691. \end_inset
  692. for cause
  693. \begin_inset Quotes erd
  694. \end_inset
  695. biopsies
  696. \begin_inset CommandInset citation
  697. LatexCommand cite
  698. key "Salomon2002,Wilkinson2006,Patel2018,Zachariah2018"
  699. literal "false"
  700. \end_inset
  701. .
  702. \end_layout
  703. \begin_layout Standard
  704. However, biopsies have a number of downsides that limit their effectiveness
  705. as a diagnostic tool.
  706. First, the need for manual inspection by a histologist means that diagnosis
  707. is subject to the biases of the particular histologist examining the biopsy
  708. \begin_inset CommandInset citation
  709. LatexCommand cite
  710. key "Kurian2014"
  711. literal "false"
  712. \end_inset
  713. .
  714. In marginal cases, two different histologists may give two different diagnoses
  715. to the same biopsy.
  716. Second, a biopsy can only evaluate if rejection is occurring in the section
  717. of the graft from which the tissue was extracted.
  718. If rejection is localized to one section of the graft and the tissue is
  719. extracted from a different section, a false negative diagnosis may result.
  720. Most importantly, extraction of tissue from a graft is invasive and is
  721. treated as an injury by the body, which results in inflammation that in
  722. turn promotes increased immune system activity.
  723. Hence, the invasiveness of biopsies severely limits the frequency with
  724. which they can safely be performed
  725. \begin_inset CommandInset citation
  726. LatexCommand cite
  727. key "Patel2018"
  728. literal "false"
  729. \end_inset
  730. .
  731. Typically, protocol biopsies are not scheduled more than about once per
  732. month
  733. \begin_inset CommandInset citation
  734. LatexCommand cite
  735. key "Wilkinson2006"
  736. literal "false"
  737. \end_inset
  738. .
  739. A less invasive diagnostic test for rejection would bring manifold benefits.
  740. Such a test would enable more frequent testing and therefore earlier detection
  741. of rejection events.
  742. In addition, having a larger pool of historical data for a given patient
  743. would make it easier to evaluate when a given test is outside the normal
  744. parameters for that specific patient, rather than relying on normal ranges
  745. for the population as a whole.
  746. Lastly, the accumulated data from more frequent tests would be a boon to
  747. the transplant research community.
  748. Beyond simply providing more data overall, the better time granularity
  749. of the tests will enable studying the progression of a rejection event
  750. on the scale of days to weeks, rather than months.
  751. \end_layout
  752. \begin_layout Subsection
  753. Memory cells are resistant to immune suppression
  754. \end_layout
  755. \begin_layout Standard
  756. \begin_inset Flex TODO Note (inline)
  757. status open
  758. \begin_layout Plain Layout
  759. Expand on costimulation required by naive cells and how memory cells differ,
  760. and mechanisms of immune suppression drugs
  761. \end_layout
  762. \end_inset
  763. \end_layout
  764. \begin_layout Standard
  765. One of the defining features of the adaptive immune system is immune memory:
  766. the ability of the immune system to recognize a previously encountered
  767. foreign antigen and respond more quickly and more strongly to that antigen
  768. in subsequent encounters
  769. \begin_inset CommandInset citation
  770. LatexCommand cite
  771. key "Murphy2012"
  772. literal "false"
  773. \end_inset
  774. .
  775. When the immune system first encounters a new antigen, the lymphocytes
  776. that respond are known as naïve cells – T-cells and B-cells that have never
  777. detected their target antigens before.
  778. Once activated by their specific antigen presented by an antigen-presenting
  779. cell in the proper co-stimulatory context, naïve cells differentiate into
  780. effector cells that carry out their respective functions in targeting and
  781. destroying the source of the foreign antigen.
  782. The dependency of activation on co-stimulation is an important feature
  783. of naïve lymphocytes that limits
  784. \begin_inset Quotes eld
  785. \end_inset
  786. false positive
  787. \begin_inset Quotes erd
  788. \end_inset
  789. immune responses, because antigen-presenting cells usually only express
  790. the proper co-stimulation after detecting evidence of an infection, such
  791. as the presence of common bacterial cell components or inflamed tissue.
  792. After the foreign antigen is cleared, most effector cells die since they
  793. are no longer needed, but some differentiate into memory cells and remain
  794. alive indefinitely.
  795. Like naïve cells, memory cells respond to detection of their specific antigen
  796. by differentiating into effector cells, ready to fight an infection.
  797. However, unlike naïve cells, memory cells do not require the same degree
  798. of co-stimulatory signaling for activation, and once activated, they proliferat
  799. e and differentiate into effector cells more quickly than naïve cells do.
  800. \end_layout
  801. \begin_layout Standard
  802. In the context of a pathogenic infection, immune memory is a major advantage,
  803. allowing an organism to rapidly fight off a previously encountered pathogen
  804. much more quickly and effectively than the first time it was encountered
  805. \begin_inset CommandInset citation
  806. LatexCommand cite
  807. key "Murphy2012"
  808. literal "false"
  809. \end_inset
  810. .
  811. However, if effector cells that recognize an antigen from an allograft
  812. are allowed to differentiate into memory cells, preventing rejection of
  813. the graft becomes much more difficult.
  814. Many immune suppression drugs work by interfering with the co-stimulation
  815. that naïve cells require in order to mount an immune response.
  816. Since memory cells do not require the same degree of co-stimulation, these
  817. drugs are not effective at suppressing an immune response that is mediated
  818. by memory cells.
  819. Secondly, because memory cells are able to mount a stronger and faster
  820. response to an antigen, all else being equal stronger immune suppression
  821. is required to prevent an immune response mediated by memory cells.
  822. \end_layout
  823. \begin_layout Standard
  824. However, immune suppression affects the entire immune system, not just cells
  825. recognizing a specific antigen, so increasing the dosage of immune suppression
  826. drugs also increases the risk of complications from a compromised immune
  827. system, such as opportunistic infections
  828. \begin_inset CommandInset citation
  829. LatexCommand cite
  830. key "Murphy2012"
  831. literal "false"
  832. \end_inset
  833. .
  834. While the differences in cell surface markers between naïve and memory
  835. cells have been fairly well characterized, the internal regulatory mechanisms
  836. that allow memory cells to respond more quickly and without co-stimulation
  837. are still poorly understood.
  838. In order to develop methods of immune suppression that either prevent the
  839. formation of memory cells or work more effectively against memory cells,
  840. a more complete understanding of the mechanisms of immune memory formation
  841. and regulation is required.
  842. \end_layout
  843. \begin_layout Subsection
  844. MSC infusion to improve transplant outcomes (prevent/delay rejection)
  845. \end_layout
  846. \begin_layout Standard
  847. One promising experimental treatment for transplant rejection involves the
  848. infusion of
  849. \begin_inset Flex Glossary Term (pl)
  850. status open
  851. \begin_layout Plain Layout
  852. MSC
  853. \end_layout
  854. \end_inset
  855. .
  856. \end_layout
  857. \begin_layout Itemize
  858. Demonstrated in mice, but not yet in primates
  859. \end_layout
  860. \begin_layout Itemize
  861. Mechanism currently unknown, but MSC are known to be immune modulatory
  862. \end_layout
  863. \begin_layout Itemize
  864. Characterize MSC response to interferon gamma
  865. \end_layout
  866. \begin_layout Itemize
  867. IFN-g is thought to stimulate their function
  868. \end_layout
  869. \begin_layout Itemize
  870. Test IFN-g treated MSC infusion as a therapy to delay graft rejection in
  871. cynomolgus monkeys
  872. \end_layout
  873. \begin_layout Itemize
  874. Monitor animals post-transplant using blood
  875. \begin_inset Flex Glossary Term
  876. status open
  877. \begin_layout Plain Layout
  878. RNA-seq
  879. \end_layout
  880. \end_inset
  881. at serial time points
  882. \end_layout
  883. \begin_layout Subsection
  884. Investigate dynamics of histone marks in CD4
  885. \begin_inset Formula $^{+}$
  886. \end_inset
  887. T-cell activation and memory
  888. \end_layout
  889. \begin_layout Standard
  890. \begin_inset Flex TODO Note (inline)
  891. status open
  892. \begin_layout Plain Layout
  893. Put this at end of intro as part of a description to structure of thesis
  894. \end_layout
  895. \end_inset
  896. \end_layout
  897. \begin_layout Itemize
  898. Previous studies have looked at single snapshots of histone marks
  899. \end_layout
  900. \begin_layout Itemize
  901. Instead, look at changes in histone marks across activation and memory
  902. \end_layout
  903. \begin_layout Subsection
  904. High-throughput sequencing and microarray technologies
  905. \end_layout
  906. \begin_layout Standard
  907. \begin_inset Flex TODO Note (inline)
  908. status open
  909. \begin_layout Plain Layout
  910. This will serve as transition to bioinf
  911. \end_layout
  912. \end_inset
  913. \end_layout
  914. \begin_layout Itemize
  915. Powerful methods for assaying gene expression and epigenetics across entire
  916. genomes
  917. \end_layout
  918. \begin_layout Itemize
  919. Proper analysis requires finding and exploiting systematic genome-wide trends
  920. \end_layout
  921. \begin_layout Section
  922. \begin_inset CommandInset label
  923. LatexCommand label
  924. name "sec:Overview-of-bioinformatic"
  925. \end_inset
  926. Overview of bioinformatic analysis methods
  927. \end_layout
  928. \begin_layout Standard
  929. \begin_inset Flex TODO Note (inline)
  930. status open
  931. \begin_layout Plain Layout
  932. Also cite somewhere: R, Bioconductor
  933. \end_layout
  934. \end_inset
  935. \end_layout
  936. \begin_layout Standard
  937. The studies presented in this work all involve the analysis of high-throughput
  938. genomic and epigenomic data.
  939. These data present many unique analysis challenges, and a wide array of
  940. software tools are available to analyze them.
  941. This section presents an overview of the most important methods used throughout
  942. the following analyses, including what problems they solve, what assumptions
  943. they make, and a basic description of how they work.
  944. \end_layout
  945. \begin_layout Subsection
  946. \begin_inset Flex Code
  947. status open
  948. \begin_layout Plain Layout
  949. Limma
  950. \end_layout
  951. \end_inset
  952. : The standard linear modeling framework for genomics
  953. \end_layout
  954. \begin_layout Standard
  955. Linear models are a generalization of the
  956. \begin_inset Formula $t$
  957. \end_inset
  958. -test and ANOVA to arbitrarily complex experimental designs
  959. \begin_inset CommandInset citation
  960. LatexCommand cite
  961. key "chambers:1992"
  962. literal "false"
  963. \end_inset
  964. .
  965. In a typical linear model, there is one dependent variable observation
  966. per sample and a large number of samples.
  967. For example, in a linear model of height as a function of age and sex,
  968. there is one height measurement per person.
  969. However, when analyzing genomic data, each sample consists of observations
  970. of thousands of dependent variables.
  971. For example, in a
  972. \begin_inset Flex Glossary Term
  973. status open
  974. \begin_layout Plain Layout
  975. RNA-seq
  976. \end_layout
  977. \end_inset
  978. experiment, the dependent variables may be the count of
  979. \begin_inset Flex Glossary Term
  980. status open
  981. \begin_layout Plain Layout
  982. RNA-seq
  983. \end_layout
  984. \end_inset
  985. reads for each annotated gene, and there are tens of thousands of genes
  986. in the human genome.
  987. Since many assays measure other things than gene expression, the abstract
  988. term
  989. \begin_inset Quotes eld
  990. \end_inset
  991. feature
  992. \begin_inset Quotes erd
  993. \end_inset
  994. is used to refer to each dependent variable being measured, which may include
  995. any genomic element, such as genes, promoters, peaks, enhancers, exons,
  996. etc.
  997. \end_layout
  998. \begin_layout Standard
  999. The simplest approach to analyzing such data would be to fit the same model
  1000. independently to each feature.
  1001. However, this is undesirable for most genomics data sets.
  1002. Genomics assays like high-throughput sequencing are expensive, and often
  1003. the process of generating the samples is also quite expensive and time-consumin
  1004. g.
  1005. This expense limits the sample sizes typically employed in genomics experiments
  1006. , so a typical genomic data set has far more features being measured than
  1007. observations (samples) per feature.
  1008. As a result, the statistical power of the linear model for each individual
  1009. feature is likewise limited by the small number of samples.
  1010. However, because thousands of features from the same set of samples are
  1011. analyzed together, there is an opportunity to improve the statistical power
  1012. of the analysis by exploiting shared patterns of variation across features.
  1013. This is the core feature of
  1014. \begin_inset Flex Code
  1015. status open
  1016. \begin_layout Plain Layout
  1017. limma
  1018. \end_layout
  1019. \end_inset
  1020. , a linear modeling framework designed for genomic data.
  1021. \begin_inset Flex Code
  1022. status open
  1023. \begin_layout Plain Layout
  1024. Limma
  1025. \end_layout
  1026. \end_inset
  1027. is typically used to analyze expression microarray data, and more recently
  1028. \begin_inset Flex Glossary Term
  1029. status open
  1030. \begin_layout Plain Layout
  1031. RNA-seq
  1032. \end_layout
  1033. \end_inset
  1034. data, but it can also be used to analyze any other data for which linear
  1035. modeling is appropriate.
  1036. \end_layout
  1037. \begin_layout Standard
  1038. The central challenge when fitting a linear model is to estimate the variance
  1039. of the data accurately.
  1040. Out of all parameters required to evaluate statistical significance of
  1041. an effect, the variance is the most difficult to estimate when sample sizes
  1042. are small.
  1043. A single shared variance could be estimated for all of the features together,
  1044. and this estimate would be very stable, in contrast to the individual feature
  1045. variance estimates.
  1046. However, this would require the assumption that all features have equal
  1047. variance, which is known to be false for most genomic data sets (for example,
  1048. some genes' expression is known to be more variable than others').
  1049. \begin_inset Flex Code
  1050. status open
  1051. \begin_layout Plain Layout
  1052. Limma
  1053. \end_layout
  1054. \end_inset
  1055. offers a compromise between these two extremes by using a method called
  1056. empirical Bayes moderation to
  1057. \begin_inset Quotes eld
  1058. \end_inset
  1059. squeeze
  1060. \begin_inset Quotes erd
  1061. \end_inset
  1062. the distribution of estimated variances toward a single common value that
  1063. represents the variance of an average feature in the data (Figure
  1064. \begin_inset CommandInset ref
  1065. LatexCommand ref
  1066. reference "fig:ebayes-example"
  1067. plural "false"
  1068. caps "false"
  1069. noprefix "false"
  1070. \end_inset
  1071. )
  1072. \begin_inset CommandInset citation
  1073. LatexCommand cite
  1074. key "Smyth2004"
  1075. literal "false"
  1076. \end_inset
  1077. .
  1078. While the individual feature variance estimates are not stable, the common
  1079. variance estimate for the entire data set is quite stable, so using a combinati
  1080. on of the two yields a variance estimate for each feature with greater precision
  1081. than the individual feature variances.
  1082. The trade-off for this improvement is that squeezing each estimated variance
  1083. toward the common value introduces some bias – the variance will be underestima
  1084. ted for features with high variance and overestimated for features with
  1085. low variance.
  1086. Essentially,
  1087. \begin_inset Flex Code
  1088. status open
  1089. \begin_layout Plain Layout
  1090. limma
  1091. \end_layout
  1092. \end_inset
  1093. assumes that extreme variances are less common than variances close to
  1094. the common value.
  1095. The squeezed variance estimates from this empirical Bayes procedure are
  1096. shown empirically to yield greater statistical power than either the individual
  1097. feature variances or the single common value.
  1098. \end_layout
  1099. \begin_layout Standard
  1100. \begin_inset Float figure
  1101. wide false
  1102. sideways false
  1103. status open
  1104. \begin_layout Plain Layout
  1105. \align center
  1106. \begin_inset Graphics
  1107. filename graphics/Intro/eBayes-CROP.pdf
  1108. lyxscale 50
  1109. width 100col%
  1110. groupId colfullwidth
  1111. \end_inset
  1112. \end_layout
  1113. \begin_layout Plain Layout
  1114. \begin_inset Caption Standard
  1115. \begin_layout Plain Layout
  1116. \begin_inset Argument 1
  1117. status collapsed
  1118. \begin_layout Plain Layout
  1119. Example of empirical Bayes squeezing of per-gene variances.
  1120. \end_layout
  1121. \end_inset
  1122. \begin_inset CommandInset label
  1123. LatexCommand label
  1124. name "fig:ebayes-example"
  1125. \end_inset
  1126. \series bold
  1127. Example of empirical Bayes squeezing of per-gene variances.
  1128. \series default
  1129. A smooth trend line (red) is fitted to the individual gene variances (light
  1130. blue) as a function of average gene abundance (logCPM).
  1131. Then the individual gene variances are
  1132. \begin_inset Quotes eld
  1133. \end_inset
  1134. squeezed
  1135. \begin_inset Quotes erd
  1136. \end_inset
  1137. toward the trend (dark blue).
  1138. \end_layout
  1139. \end_inset
  1140. \end_layout
  1141. \begin_layout Plain Layout
  1142. \end_layout
  1143. \end_inset
  1144. \end_layout
  1145. \begin_layout Standard
  1146. On top of this core framework,
  1147. \begin_inset Flex Code
  1148. status open
  1149. \begin_layout Plain Layout
  1150. limma
  1151. \end_layout
  1152. \end_inset
  1153. also implements many other enhancements that, further relax the assumptions
  1154. of the model and extend the scope of what kinds of data it can analyze.
  1155. Instead of squeezing toward a single common variance value,
  1156. \begin_inset Flex Code
  1157. status open
  1158. \begin_layout Plain Layout
  1159. limma
  1160. \end_layout
  1161. \end_inset
  1162. can model the common variance as a function of a covariate, such as average
  1163. expression
  1164. \begin_inset CommandInset citation
  1165. LatexCommand cite
  1166. key "Law2013"
  1167. literal "false"
  1168. \end_inset
  1169. .
  1170. This is essential for
  1171. \begin_inset Flex Glossary Term
  1172. status open
  1173. \begin_layout Plain Layout
  1174. RNA-seq
  1175. \end_layout
  1176. \end_inset
  1177. data, where higher gene counts yield more precise expression measurements
  1178. and therefore smaller variances than low-count genes.
  1179. While linear models typically assume that all samples have equal variance,
  1180. \begin_inset Flex Code
  1181. status open
  1182. \begin_layout Plain Layout
  1183. limma
  1184. \end_layout
  1185. \end_inset
  1186. is able to relax this assumption by identifying and down-weighting samples
  1187. that diverge more strongly from the linear model across many features
  1188. \begin_inset CommandInset citation
  1189. LatexCommand cite
  1190. key "Ritchie2006,Liu2015"
  1191. literal "false"
  1192. \end_inset
  1193. .
  1194. In addition,
  1195. \begin_inset Flex Code
  1196. status open
  1197. \begin_layout Plain Layout
  1198. limma
  1199. \end_layout
  1200. \end_inset
  1201. is also able to fit simple mixed models incorporating one random effect
  1202. in addition to the fixed effects represented by an ordinary linear model
  1203. \begin_inset CommandInset citation
  1204. LatexCommand cite
  1205. key "Smyth2005a"
  1206. literal "false"
  1207. \end_inset
  1208. .
  1209. Once again,
  1210. \begin_inset Flex Code
  1211. status open
  1212. \begin_layout Plain Layout
  1213. limma
  1214. \end_layout
  1215. \end_inset
  1216. shares information between features to obtain a robust estimate for the
  1217. random effect correlation.
  1218. \end_layout
  1219. \begin_layout Subsection
  1220. \begin_inset Flex Code
  1221. status open
  1222. \begin_layout Plain Layout
  1223. edgeR
  1224. \end_layout
  1225. \end_inset
  1226. provides
  1227. \begin_inset Flex Code
  1228. status open
  1229. \begin_layout Plain Layout
  1230. limma
  1231. \end_layout
  1232. \end_inset
  1233. -like analysis features for count data
  1234. \end_layout
  1235. \begin_layout Standard
  1236. Although
  1237. \begin_inset Flex Code
  1238. status open
  1239. \begin_layout Plain Layout
  1240. limma
  1241. \end_layout
  1242. \end_inset
  1243. can be applied to read counts from
  1244. \begin_inset Flex Glossary Term
  1245. status open
  1246. \begin_layout Plain Layout
  1247. RNA-seq
  1248. \end_layout
  1249. \end_inset
  1250. data, it is less suitable for counts from
  1251. \begin_inset Flex Glossary Term
  1252. status open
  1253. \begin_layout Plain Layout
  1254. ChIP-seq
  1255. \end_layout
  1256. \end_inset
  1257. and other sources, which tend to be much smaller and therefore violate
  1258. the assumption of a normal distribution more severely.
  1259. For all count-based data, the
  1260. \begin_inset Flex Code
  1261. status open
  1262. \begin_layout Plain Layout
  1263. edgeR
  1264. \end_layout
  1265. \end_inset
  1266. package works similarly to
  1267. \begin_inset Flex Code
  1268. status open
  1269. \begin_layout Plain Layout
  1270. limma
  1271. \end_layout
  1272. \end_inset
  1273. , but uses a
  1274. \begin_inset Flex Glossary Term
  1275. status open
  1276. \begin_layout Plain Layout
  1277. GLM
  1278. \end_layout
  1279. \end_inset
  1280. instead of a linear model.
  1281. Relative to a linear model, a
  1282. \begin_inset Flex Glossary Term
  1283. status open
  1284. \begin_layout Plain Layout
  1285. GLM
  1286. \end_layout
  1287. \end_inset
  1288. gains flexibility by relaxing several assumptions, the most important of
  1289. which is the assumption of normally distributed errors.
  1290. This allows the
  1291. \begin_inset Flex Glossary Term
  1292. status open
  1293. \begin_layout Plain Layout
  1294. GLM
  1295. \end_layout
  1296. \end_inset
  1297. in
  1298. \begin_inset Flex Code
  1299. status open
  1300. \begin_layout Plain Layout
  1301. edgeR
  1302. \end_layout
  1303. \end_inset
  1304. to model the counts directly using a
  1305. \begin_inset Flex Glossary Term
  1306. status open
  1307. \begin_layout Plain Layout
  1308. NB
  1309. \end_layout
  1310. \end_inset
  1311. distribution rather than modeling the normalized log counts using a normal
  1312. distribution as
  1313. \begin_inset Flex Code
  1314. status open
  1315. \begin_layout Plain Layout
  1316. limma
  1317. \end_layout
  1318. \end_inset
  1319. does
  1320. \begin_inset CommandInset citation
  1321. LatexCommand cite
  1322. key "Chen2014,McCarthy2012,Robinson2010a"
  1323. literal "false"
  1324. \end_inset
  1325. .
  1326. \end_layout
  1327. \begin_layout Standard
  1328. The
  1329. \begin_inset Flex Glossary Term
  1330. status open
  1331. \begin_layout Plain Layout
  1332. NB
  1333. \end_layout
  1334. \end_inset
  1335. distribution is a good fit for count data because it can be derived as
  1336. a gamma-distributed mixture of Poisson distributions.
  1337. The reads in an
  1338. \begin_inset Flex Glossary Term
  1339. status open
  1340. \begin_layout Plain Layout
  1341. RNA-seq
  1342. \end_layout
  1343. \end_inset
  1344. sample are assumed to be sampled from a much larger population, such that
  1345. the sampling process does not significantly affect the proportions.
  1346. Under this assumption, a gene's read count in an
  1347. \begin_inset Flex Glossary Term
  1348. status open
  1349. \begin_layout Plain Layout
  1350. RNA-seq
  1351. \end_layout
  1352. \end_inset
  1353. sample is distributed as
  1354. \begin_inset Formula $\mathrm{Binomial}(n,p)$
  1355. \end_inset
  1356. , where
  1357. \begin_inset Formula $n$
  1358. \end_inset
  1359. is the total number of reads sequenced from the sample and
  1360. \begin_inset Formula $p$
  1361. \end_inset
  1362. is the proportion of total fragments in the sample derived from that gene.
  1363. When
  1364. \begin_inset Formula $n$
  1365. \end_inset
  1366. is large and
  1367. \begin_inset Formula $p$
  1368. \end_inset
  1369. is small, a
  1370. \begin_inset Formula $\mathrm{Binomial}(n,p)$
  1371. \end_inset
  1372. distribution is well-approximated by
  1373. \begin_inset Formula $\mathrm{Poisson}(np)$
  1374. \end_inset
  1375. .
  1376. Hence, if multiple sequencing runs are performed on the same
  1377. \begin_inset Flex Glossary Term
  1378. status open
  1379. \begin_layout Plain Layout
  1380. RNA-seq
  1381. \end_layout
  1382. \end_inset
  1383. sample (with the same gene mixing proportions each time), each gene's read
  1384. count is expected to follow a Poisson distribution.
  1385. If the abundance of a gene,
  1386. \begin_inset Formula $p,$
  1387. \end_inset
  1388. varies across biological replicates according to a gamma distribution,
  1389. and
  1390. \begin_inset Formula $n$
  1391. \end_inset
  1392. is held constant, then the result is a gamma-distributed mixture of Poisson
  1393. distributions, which is equivalent to the
  1394. \begin_inset Flex Glossary Term
  1395. status open
  1396. \begin_layout Plain Layout
  1397. NB
  1398. \end_layout
  1399. \end_inset
  1400. distribution.
  1401. The assumption of a gamma distribution for the mixing weights is arbitrary,
  1402. motivated by the convenience of the numerically tractable
  1403. \begin_inset Flex Glossary Term
  1404. status open
  1405. \begin_layout Plain Layout
  1406. NB
  1407. \end_layout
  1408. \end_inset
  1409. distribution and the need to select
  1410. \emph on
  1411. some
  1412. \emph default
  1413. distribution, since the true shape of the distribution of biological variance
  1414. is unknown.
  1415. \end_layout
  1416. \begin_layout Standard
  1417. Thus,
  1418. \begin_inset Flex Code
  1419. status open
  1420. \begin_layout Plain Layout
  1421. edgeR
  1422. \end_layout
  1423. \end_inset
  1424. 's use of the
  1425. \begin_inset Flex Glossary Term
  1426. status open
  1427. \begin_layout Plain Layout
  1428. NB
  1429. \end_layout
  1430. \end_inset
  1431. is equivalent to an
  1432. \emph on
  1433. a priori
  1434. \emph default
  1435. assumption that the variation in gene abundances between replicates follows
  1436. a gamma distribution.
  1437. The gamma shape parameter in the context of the
  1438. \begin_inset Flex Glossary Term
  1439. status open
  1440. \begin_layout Plain Layout
  1441. NB
  1442. \end_layout
  1443. \end_inset
  1444. is called the dispersion, and the square root of this dispersion is referred
  1445. to as the
  1446. \begin_inset Flex Glossary Term
  1447. status open
  1448. \begin_layout Plain Layout
  1449. BCV
  1450. \end_layout
  1451. \end_inset
  1452. , since it represents the variability in abundance that was present in the
  1453. biological samples prior to the Poisson
  1454. \begin_inset Quotes eld
  1455. \end_inset
  1456. noise
  1457. \begin_inset Quotes erd
  1458. \end_inset
  1459. that was generated by the random sampling of reads in proportion to feature
  1460. abundances.
  1461. Like
  1462. \begin_inset Flex Code
  1463. status open
  1464. \begin_layout Plain Layout
  1465. limma
  1466. \end_layout
  1467. \end_inset
  1468. ,
  1469. \begin_inset Flex Code
  1470. status open
  1471. \begin_layout Plain Layout
  1472. edgeR
  1473. \end_layout
  1474. \end_inset
  1475. estimates the
  1476. \begin_inset Flex Glossary Term
  1477. status open
  1478. \begin_layout Plain Layout
  1479. BCV
  1480. \end_layout
  1481. \end_inset
  1482. for each feature using an empirical Bayes procedure that represents a compromis
  1483. e between per-feature dispersions and a single pooled dispersion estimate
  1484. shared across all features.
  1485. For differential abundance testing,
  1486. \begin_inset Flex Code
  1487. status open
  1488. \begin_layout Plain Layout
  1489. edgeR
  1490. \end_layout
  1491. \end_inset
  1492. offers a likelihood ratio test based on the
  1493. \begin_inset Flex Glossary Term
  1494. status open
  1495. \begin_layout Plain Layout
  1496. NB
  1497. \end_layout
  1498. \end_inset
  1499. \begin_inset Flex Glossary Term
  1500. status open
  1501. \begin_layout Plain Layout
  1502. GLM
  1503. \end_layout
  1504. \end_inset
  1505. .
  1506. However, this test assumes the dispersion parameter is known exactly rather
  1507. than estimated from the data, which can result in overstating the significance
  1508. of differential abundance results.
  1509. More recently, a quasi-likelihood test has been introduced that properly
  1510. factors the uncertainty in dispersion estimation into the estimates of
  1511. statistical significance, and this test is recommended over the likelihood
  1512. ratio test in most cases
  1513. \begin_inset CommandInset citation
  1514. LatexCommand cite
  1515. key "Lund2012"
  1516. literal "false"
  1517. \end_inset
  1518. .
  1519. \end_layout
  1520. \begin_layout Subsection
  1521. ChIP-seq Peak calling
  1522. \end_layout
  1523. \begin_layout Standard
  1524. Unlike
  1525. \begin_inset Flex Glossary Term
  1526. status open
  1527. \begin_layout Plain Layout
  1528. RNA-seq
  1529. \end_layout
  1530. \end_inset
  1531. data, in which gene annotations provide a well-defined set of discrete
  1532. genomic regions in which to count reads,
  1533. \begin_inset Flex Glossary Term
  1534. status open
  1535. \begin_layout Plain Layout
  1536. ChIP-seq
  1537. \end_layout
  1538. \end_inset
  1539. reads can potentially occur anywhere in the genome.
  1540. However, most genome regions will not contain significant
  1541. \begin_inset Flex Glossary Term
  1542. status open
  1543. \begin_layout Plain Layout
  1544. ChIP-seq
  1545. \end_layout
  1546. \end_inset
  1547. read coverage, and analyzing every position in the entire genome is statistical
  1548. ly and computationally infeasible, so it is necessary to identify regions
  1549. of interest inside which
  1550. \begin_inset Flex Glossary Term
  1551. status open
  1552. \begin_layout Plain Layout
  1553. ChIP-seq
  1554. \end_layout
  1555. \end_inset
  1556. reads will be counted and analyzed.
  1557. One option is to define a set of interesting regions
  1558. \emph on
  1559. a priori
  1560. \emph default
  1561. , for example by defining a promoter region for each annotated gene.
  1562. However, it is also possible to use the
  1563. \begin_inset Flex Glossary Term
  1564. status open
  1565. \begin_layout Plain Layout
  1566. ChIP-seq
  1567. \end_layout
  1568. \end_inset
  1569. data itself to identify regions with
  1570. \begin_inset Flex Glossary Term
  1571. status open
  1572. \begin_layout Plain Layout
  1573. ChIP-seq
  1574. \end_layout
  1575. \end_inset
  1576. read coverage significantly above the background level, known as peaks.
  1577. \end_layout
  1578. \begin_layout Standard
  1579. The challenge in peak calling is that the immunoprecipitation step is not
  1580. 100% selective, so some fraction of reads are
  1581. \emph on
  1582. not
  1583. \emph default
  1584. derived from DNA fragments that were bound by the immunoprecipitated protein.
  1585. These are referred to as background reads.
  1586. Biases in amplification and sequencing, as well as the aforementioned Poisson
  1587. randomness of the sequencing itself, can cause fluctuations in the background
  1588. level of reads the resemble peaks, and the true peaks must be distinguished
  1589. from these.
  1590. It is common to sequence the input to the ChIP-seq reaction as well as
  1591. the immunoprecipitated sample in order to aid in estimating the fluctuations
  1592. in background level across the genome.
  1593. \end_layout
  1594. \begin_layout Standard
  1595. There are generally two kinds of peaks that can be identified: narrow peaks
  1596. and broadly enriched regions.
  1597. Proteins like transcription factors that bind specific sites in the genome
  1598. typically show most of their
  1599. \begin_inset Flex Glossary Term
  1600. status open
  1601. \begin_layout Plain Layout
  1602. ChIP-seq
  1603. \end_layout
  1604. \end_inset
  1605. read coverage at these specific sites and very little coverage anywhere
  1606. else.
  1607. Because the footprint of the protein is consistent wherever it binds, each
  1608. peak has a consistent width, typically tens to hundreds of base pairs,
  1609. representing the length of DNA that it binds to.
  1610. Algorithms like
  1611. \begin_inset Flex Glossary Term
  1612. status open
  1613. \begin_layout Plain Layout
  1614. MACS
  1615. \end_layout
  1616. \end_inset
  1617. exploit this pattern to identify specific loci at which such
  1618. \begin_inset Quotes eld
  1619. \end_inset
  1620. narrow peaks
  1621. \begin_inset Quotes erd
  1622. \end_inset
  1623. occur by looking for the characteristic peak shape in the
  1624. \begin_inset Flex Glossary Term
  1625. status open
  1626. \begin_layout Plain Layout
  1627. ChIP-seq
  1628. \end_layout
  1629. \end_inset
  1630. coverage rising above the surrounding background coverage
  1631. \begin_inset CommandInset citation
  1632. LatexCommand cite
  1633. key "Zhang2008"
  1634. literal "false"
  1635. \end_inset
  1636. .
  1637. In contrast, some proteins, chief among them histones, do not bind only
  1638. at a small number of specific sites, but rather bind potentially almost
  1639. everywhere in the entire genome.
  1640. When looking at histone marks, adjacent histones tend to be similarly marked,
  1641. and a given mark may be present on an arbitrary number of consecutive histones
  1642. along the genome.
  1643. Hence, there is no consistent
  1644. \begin_inset Quotes eld
  1645. \end_inset
  1646. footprint size
  1647. \begin_inset Quotes erd
  1648. \end_inset
  1649. for
  1650. \begin_inset Flex Glossary Term
  1651. status open
  1652. \begin_layout Plain Layout
  1653. ChIP-seq
  1654. \end_layout
  1655. \end_inset
  1656. peaks based on histone marks, and peaks typically span many histones.
  1657. Hence, typical peaks span many hundreds or even thousands of base pairs.
  1658. Instead of identifying specific loci of strong enrichment, algorithms like
  1659. \begin_inset Flex Glossary Term
  1660. status open
  1661. \begin_layout Plain Layout
  1662. SICER
  1663. \end_layout
  1664. \end_inset
  1665. assume that peaks are represented in the
  1666. \begin_inset Flex Glossary Term
  1667. status open
  1668. \begin_layout Plain Layout
  1669. ChIP-seq
  1670. \end_layout
  1671. \end_inset
  1672. data by modest enrichment above background occurring across broad regions,
  1673. and they attempt to identify the extent of those regions
  1674. \begin_inset CommandInset citation
  1675. LatexCommand cite
  1676. key "Zang2009"
  1677. literal "false"
  1678. \end_inset
  1679. .
  1680. \end_layout
  1681. \begin_layout Standard
  1682. Regardless of the type of peak identified, it is important to identify peaks
  1683. that occur consistently across biological replicates.
  1684. The
  1685. \begin_inset Flex Glossary Term
  1686. status open
  1687. \begin_layout Plain Layout
  1688. ENCODE
  1689. \end_layout
  1690. \end_inset
  1691. project has developed a method called
  1692. \begin_inset Flex Glossary Term
  1693. status open
  1694. \begin_layout Plain Layout
  1695. IDR
  1696. \end_layout
  1697. \end_inset
  1698. for this purpose
  1699. \begin_inset CommandInset citation
  1700. LatexCommand cite
  1701. key "Li2006"
  1702. literal "false"
  1703. \end_inset
  1704. .
  1705. The
  1706. \begin_inset Flex Glossary Term
  1707. status open
  1708. \begin_layout Plain Layout
  1709. IDR
  1710. \end_layout
  1711. \end_inset
  1712. is defined as the probability that a peak identified in one biological
  1713. replicate will
  1714. \emph on
  1715. not
  1716. \emph default
  1717. also be identified in a second replicate.
  1718. Where the more familiar false discovery rate measures the degree of corresponde
  1719. nce between a data-derived ranked list and the (unknown) true list of significan
  1720. t features,
  1721. \begin_inset Flex Glossary Term
  1722. status open
  1723. \begin_layout Plain Layout
  1724. IDR
  1725. \end_layout
  1726. \end_inset
  1727. instead measures the degree of correspondence between two ranked lists
  1728. derived from different data.
  1729. \begin_inset Flex Glossary Term
  1730. status open
  1731. \begin_layout Plain Layout
  1732. IDR
  1733. \end_layout
  1734. \end_inset
  1735. assumes that the highest-ranked features are
  1736. \begin_inset Quotes eld
  1737. \end_inset
  1738. signal
  1739. \begin_inset Quotes erd
  1740. \end_inset
  1741. peaks that tend to be listed in the same order in both lists, while the
  1742. lowest-ranked features are essentially noise peaks, listed in random order
  1743. with no correspondence between the lists.
  1744. \begin_inset Flex Glossary Term (Capital)
  1745. status open
  1746. \begin_layout Plain Layout
  1747. IDR
  1748. \end_layout
  1749. \end_inset
  1750. attempts to locate the
  1751. \begin_inset Quotes eld
  1752. \end_inset
  1753. crossover point
  1754. \begin_inset Quotes erd
  1755. \end_inset
  1756. between the signal and the noise by determining how far down the list the
  1757. rank consistency breaks down into randomness (Figure
  1758. \begin_inset CommandInset ref
  1759. LatexCommand ref
  1760. reference "fig:Example-IDR"
  1761. plural "false"
  1762. caps "false"
  1763. noprefix "false"
  1764. \end_inset
  1765. ).
  1766. \end_layout
  1767. \begin_layout Standard
  1768. \begin_inset Float figure
  1769. wide false
  1770. sideways false
  1771. status open
  1772. \begin_layout Plain Layout
  1773. \align center
  1774. \begin_inset Graphics
  1775. filename graphics/CD4-csaw/IDR/D4659vsD5053_epic-PAGE1-CROP.pdf
  1776. lyxscale 50
  1777. width 100col%
  1778. groupId colfullwidth
  1779. \end_inset
  1780. \end_layout
  1781. \begin_layout Plain Layout
  1782. \begin_inset Caption Standard
  1783. \begin_layout Plain Layout
  1784. \begin_inset Argument 1
  1785. status collapsed
  1786. \begin_layout Plain Layout
  1787. Example IDR consistency plot.
  1788. \end_layout
  1789. \end_inset
  1790. \begin_inset CommandInset label
  1791. LatexCommand label
  1792. name "fig:Example-IDR"
  1793. \end_inset
  1794. \series bold
  1795. Example IDR consistency plot.
  1796. \series default
  1797. Peak calls in two replicates are ranked from highest score (top and right)
  1798. to lowest score (bottom and left).
  1799. IDR identifies reproducible peaks, which rank highly in both replicates
  1800. (light blue), separating them from
  1801. \begin_inset Quotes eld
  1802. \end_inset
  1803. noise
  1804. \begin_inset Quotes erd
  1805. \end_inset
  1806. peak calls whose ranking is not reproducible between replicates (dark blue).
  1807. \end_layout
  1808. \end_inset
  1809. \end_layout
  1810. \begin_layout Plain Layout
  1811. \end_layout
  1812. \end_inset
  1813. \end_layout
  1814. \begin_layout Standard
  1815. In addition to other considerations, if called peaks are to be used as regions
  1816. of interest for differential abundance analysis, then care must be taken
  1817. to call peaks in a way that is blind to differential abundance between
  1818. experimental conditions, or else the statistical significance calculations
  1819. for differential abundance will overstate their confidence in the results.
  1820. The
  1821. \begin_inset Flex Code
  1822. status open
  1823. \begin_layout Plain Layout
  1824. csaw
  1825. \end_layout
  1826. \end_inset
  1827. package provides guidelines for calling peaks in this way: peaks are called
  1828. based on a combination of all
  1829. \begin_inset Flex Glossary Term
  1830. status open
  1831. \begin_layout Plain Layout
  1832. ChIP-seq
  1833. \end_layout
  1834. \end_inset
  1835. reads from all experimental conditions, so that the identified peaks are
  1836. based on the average abundance across all conditions, which is independent
  1837. of any differential abundance between conditions
  1838. \begin_inset CommandInset citation
  1839. LatexCommand cite
  1840. key "Lun2015a"
  1841. literal "false"
  1842. \end_inset
  1843. .
  1844. \end_layout
  1845. \begin_layout Subsection
  1846. Normalization of high-throughput data is non-trivial and application-dependent
  1847. \end_layout
  1848. \begin_layout Standard
  1849. High-throughput data sets invariably require some kind of normalization
  1850. before further analysis can be conducted.
  1851. In general, the goal of normalization is to remove effects in the data
  1852. that are caused by technical factors that have nothing to do with the biology
  1853. being studied.
  1854. \end_layout
  1855. \begin_layout Standard
  1856. For Affymetrix expression arrays, the standard normalization algorithm used
  1857. in most analyses is
  1858. \begin_inset Flex Glossary Term
  1859. status open
  1860. \begin_layout Plain Layout
  1861. RMA
  1862. \end_layout
  1863. \end_inset
  1864. \begin_inset CommandInset citation
  1865. LatexCommand cite
  1866. key "Irizarry2003a"
  1867. literal "false"
  1868. \end_inset
  1869. .
  1870. \begin_inset Flex Glossary Term
  1871. status open
  1872. \begin_layout Plain Layout
  1873. RMA
  1874. \end_layout
  1875. \end_inset
  1876. is designed with the assumption that some fraction of probes on each array
  1877. will be artifactual and takes advantage of the fact that each gene is represent
  1878. ed by multiple probes by implementing normalization and summarization steps
  1879. that are robust against outlier probes.
  1880. However,
  1881. \begin_inset Flex Glossary Term
  1882. status open
  1883. \begin_layout Plain Layout
  1884. RMA
  1885. \end_layout
  1886. \end_inset
  1887. uses the probe intensities of all arrays in the data set in the normalization
  1888. of each individual array, meaning that the normalized expression values
  1889. in each array depend on every array in the data set, and will necessarily
  1890. change each time an array is added or removed from the data set.
  1891. If this is undesirable,
  1892. \begin_inset Flex Glossary Term
  1893. status open
  1894. \begin_layout Plain Layout
  1895. fRMA
  1896. \end_layout
  1897. \end_inset
  1898. implements a variant of
  1899. \begin_inset Flex Glossary Term
  1900. status open
  1901. \begin_layout Plain Layout
  1902. RMA
  1903. \end_layout
  1904. \end_inset
  1905. where the relevant distributional parameters are learned from a large reference
  1906. set of diverse public array data sets and then
  1907. \begin_inset Quotes eld
  1908. \end_inset
  1909. frozen
  1910. \begin_inset Quotes erd
  1911. \end_inset
  1912. , so that each array is effectively normalized against this frozen reference
  1913. set rather than the other arrays in the data set under study
  1914. \begin_inset CommandInset citation
  1915. LatexCommand cite
  1916. key "McCall2010"
  1917. literal "false"
  1918. \end_inset
  1919. .
  1920. Other available array normalization methods considered include dChip,
  1921. \begin_inset Flex Glossary Term
  1922. status open
  1923. \begin_layout Plain Layout
  1924. GRSN
  1925. \end_layout
  1926. \end_inset
  1927. , and
  1928. \begin_inset Flex Glossary Term
  1929. status open
  1930. \begin_layout Plain Layout
  1931. SCAN
  1932. \end_layout
  1933. \end_inset
  1934. \begin_inset CommandInset citation
  1935. LatexCommand cite
  1936. key "Li2001,Pelz2008,Piccolo2012"
  1937. literal "false"
  1938. \end_inset
  1939. .
  1940. \end_layout
  1941. \begin_layout Standard
  1942. In contrast, high-throughput sequencing data present very different normalizatio
  1943. n challenges.
  1944. The simplest case is
  1945. \begin_inset Flex Glossary Term
  1946. status open
  1947. \begin_layout Plain Layout
  1948. RNA-seq
  1949. \end_layout
  1950. \end_inset
  1951. in which read counts are obtained for a set of gene annotations, yielding
  1952. a matrix of counts with rows representing genes and columns representing
  1953. samples.
  1954. Because
  1955. \begin_inset Flex Glossary Term
  1956. status open
  1957. \begin_layout Plain Layout
  1958. RNA-seq
  1959. \end_layout
  1960. \end_inset
  1961. approximates a process of sampling from a population with replacement,
  1962. each gene's count is only interpretable as a fraction of the total reads
  1963. for that sample.
  1964. For that reason,
  1965. \begin_inset Flex Glossary Term
  1966. status open
  1967. \begin_layout Plain Layout
  1968. RNA-seq
  1969. \end_layout
  1970. \end_inset
  1971. abundances are often reported as
  1972. \begin_inset Flex Glossary Term
  1973. status open
  1974. \begin_layout Plain Layout
  1975. CPM
  1976. \end_layout
  1977. \end_inset
  1978. .
  1979. Furthermore, if the abundance of a single gene increases, then in order
  1980. for its fraction of the total reads to increase, all other genes' fractions
  1981. must decrease to accommodate it.
  1982. This effect is known as composition bias, and it is an artifact of the
  1983. read sampling process that has nothing to do with the biology of the samples
  1984. and must therefore be normalized out.
  1985. The most commonly used methods to normalize for composition bias in
  1986. \begin_inset Flex Glossary Term
  1987. status open
  1988. \begin_layout Plain Layout
  1989. RNA-seq
  1990. \end_layout
  1991. \end_inset
  1992. data seek to equalize the average gene abundance across samples, under
  1993. the assumption that the average gene is likely not changing
  1994. \begin_inset CommandInset citation
  1995. LatexCommand cite
  1996. key "Robinson2010,Anders2010"
  1997. literal "false"
  1998. \end_inset
  1999. .
  2000. The effect of such normalizations is to center the distribution of
  2001. \begin_inset Flex Glossary Term (pl)
  2002. status open
  2003. \begin_layout Plain Layout
  2004. logFC
  2005. \end_layout
  2006. \end_inset
  2007. at zero.
  2008. Note that if a true global difference in gene expression is present in
  2009. the data, this difference will be normalized out as well, since it is indisting
  2010. uishable from composition bias.
  2011. In other words,
  2012. \begin_inset Flex Glossary Term
  2013. status open
  2014. \begin_layout Plain Layout
  2015. RNA-seq
  2016. \end_layout
  2017. \end_inset
  2018. cannot measure absolute gene expression, only gene expression as a fraction
  2019. of total reads.
  2020. \end_layout
  2021. \begin_layout Standard
  2022. In
  2023. \begin_inset Flex Glossary Term
  2024. status open
  2025. \begin_layout Plain Layout
  2026. ChIP-seq
  2027. \end_layout
  2028. \end_inset
  2029. data, normalization is not as straightforward.
  2030. The
  2031. \begin_inset Flex Code
  2032. status open
  2033. \begin_layout Plain Layout
  2034. csaw
  2035. \end_layout
  2036. \end_inset
  2037. package implements several different normalization strategies and provides
  2038. guidance on when to use each one
  2039. \begin_inset CommandInset citation
  2040. LatexCommand cite
  2041. key "Lun2015a"
  2042. literal "false"
  2043. \end_inset
  2044. .
  2045. Briefly, a typical
  2046. \begin_inset Flex Glossary Term
  2047. status open
  2048. \begin_layout Plain Layout
  2049. ChIP-seq
  2050. \end_layout
  2051. \end_inset
  2052. sample has a bimodal distribution of read counts: a low-abundance mode
  2053. representing background regions and a high-abundance mode representing
  2054. signal regions.
  2055. This offers two mutually incompatible normalization strategies: equalizing
  2056. background coverage or equalizing signal coverage (Figure
  2057. \begin_inset CommandInset ref
  2058. LatexCommand ref
  2059. reference "fig:chipseq-norm-example"
  2060. plural "false"
  2061. caps "false"
  2062. noprefix "false"
  2063. \end_inset
  2064. ).
  2065. If the experiment is well controlled and ChIP efficiency is known to be
  2066. consistent across all samples, then normalizing the background coverage
  2067. to be equal across all samples is a reasonable strategy.
  2068. If this is not a safe assumption, then the preferred strategy is to normalize
  2069. the signal regions in a way similar to
  2070. \begin_inset Flex Glossary Term
  2071. status open
  2072. \begin_layout Plain Layout
  2073. RNA-seq
  2074. \end_layout
  2075. \end_inset
  2076. data by assuming that the average signal region is not changing abundance
  2077. between samples.
  2078. Beyond this, if a
  2079. \begin_inset Flex Glossary Term
  2080. status open
  2081. \begin_layout Plain Layout
  2082. ChIP-seq
  2083. \end_layout
  2084. \end_inset
  2085. experiment has a more complicated structure that doesn't show the typical
  2086. bimodal count distribution, it may be necessary to implement a normalization
  2087. as a smooth function of abundance.
  2088. However, this strategy makes a much stronger assumption about the data:
  2089. that the average
  2090. \begin_inset Flex Glossary Term
  2091. status open
  2092. \begin_layout Plain Layout
  2093. logFC
  2094. \end_layout
  2095. \end_inset
  2096. is zero across all abundance levels.
  2097. Hence, the simpler scaling normalization based on background or signal
  2098. regions are generally preferred whenever possible.
  2099. \end_layout
  2100. \begin_layout Standard
  2101. \begin_inset Float figure
  2102. wide false
  2103. sideways false
  2104. status open
  2105. \begin_layout Plain Layout
  2106. \align center
  2107. \begin_inset Graphics
  2108. filename graphics/CD4-csaw/ChIP-seq/H3K4me2-sample-MAplot-bins-CROP.png
  2109. lyxscale 25
  2110. width 100col%
  2111. groupId colwidth-raster
  2112. \end_inset
  2113. \end_layout
  2114. \begin_layout Plain Layout
  2115. \begin_inset Caption Standard
  2116. \begin_layout Plain Layout
  2117. \begin_inset Argument 1
  2118. status collapsed
  2119. \begin_layout Plain Layout
  2120. Example MA plot of ChIP-seq read counts in 10kb bins for two arbitrary samples.
  2121. \end_layout
  2122. \end_inset
  2123. \begin_inset CommandInset label
  2124. LatexCommand label
  2125. name "fig:chipseq-norm-example"
  2126. \end_inset
  2127. \series bold
  2128. Example MA plot of ChIP-seq read counts in 10kb bins for two arbitrary samples.
  2129. \series default
  2130. The distribution of bins is bimodal along the x axis (average abundance),
  2131. with the left mode representing
  2132. \begin_inset Quotes eld
  2133. \end_inset
  2134. background
  2135. \begin_inset Quotes erd
  2136. \end_inset
  2137. regions with no protein binding and the right mode representing bound regions.
  2138. The modes are also separated on the y axis (logFC), motivating two conflicting
  2139. normalization strategies: background normalization (red) and signal normalizati
  2140. on (blue and green, two similar signal normalizations).
  2141. \end_layout
  2142. \end_inset
  2143. \end_layout
  2144. \end_inset
  2145. \end_layout
  2146. \begin_layout Subsection
  2147. ComBat and SVA for correction of known and unknown batch effects
  2148. \end_layout
  2149. \begin_layout Standard
  2150. In addition to well-understood effects that can be easily normalized out,
  2151. a data set often contains confounding biological effects that must be accounted
  2152. for in the modeling step.
  2153. For instance, in an experiment with pre-treatment and post-treatment samples
  2154. of cells from several different donors, donor variability represents a
  2155. known batch effect.
  2156. The most straightforward correction for known batches is to estimate the
  2157. mean for each batch independently and subtract out the differences, so
  2158. that all batches have identical means for each feature.
  2159. However, as with variance estimation, estimating the differences in batch
  2160. means is not necessarily robust at the feature level, so the ComBat method
  2161. adds empirical Bayes squeezing of the batch mean differences toward a common
  2162. value, analogous to
  2163. \begin_inset Flex Code
  2164. status open
  2165. \begin_layout Plain Layout
  2166. limma
  2167. \end_layout
  2168. \end_inset
  2169. 's empirical Bayes squeezing of feature variance estimates
  2170. \begin_inset CommandInset citation
  2171. LatexCommand cite
  2172. key "Johnson2007"
  2173. literal "false"
  2174. \end_inset
  2175. .
  2176. Effectively, ComBat assumes that modest differences between batch means
  2177. are real batch effects, but extreme differences between batch means are
  2178. more likely to be the result of outlier observations that happen to line
  2179. up with the batches rather than a genuine batch effect.
  2180. The result is a batch correction that is more robust against outliers than
  2181. simple subtraction of mean differences.
  2182. \end_layout
  2183. \begin_layout Standard
  2184. In some data sets, unknown batch effects may be present due to inherent
  2185. variability in the data, either caused by technical or biological effects.
  2186. Examples of unknown batch effects include variations in enrichment efficiency
  2187. between
  2188. \begin_inset Flex Glossary Term
  2189. status open
  2190. \begin_layout Plain Layout
  2191. ChIP-seq
  2192. \end_layout
  2193. \end_inset
  2194. samples, variations in populations of different cell types, and the effects
  2195. of uncontrolled environmental factors on gene expression in humans or live
  2196. animals.
  2197. In an ordinary linear model context, unknown batch effects cannot be inferred
  2198. and must be treated as random noise.
  2199. However, in high-throughput experiments, once again information can be
  2200. shared across features to identify patterns of un-modeled variation that
  2201. are repeated in many features.
  2202. One attractive strategy would be to perform
  2203. \begin_inset Flex Glossary Term
  2204. status open
  2205. \begin_layout Plain Layout
  2206. SVD
  2207. \end_layout
  2208. \end_inset
  2209. on the matrix of linear model residuals (which contain all the un-modeled
  2210. variation in the data) and take the first few singular vectors as batch
  2211. effects.
  2212. While this can be effective, it makes the unreasonable assumption that
  2213. all batch effects are completely uncorrelated with any of the effects being
  2214. modeled.
  2215. \begin_inset Flex Glossary Term
  2216. status open
  2217. \begin_layout Plain Layout
  2218. SVA
  2219. \end_layout
  2220. \end_inset
  2221. starts with this approach, but takes some additional steps to identify
  2222. batch effects in the full data that are both highly correlated with the
  2223. singular vectors in the residuals and least correlated with the effects
  2224. of interest
  2225. \begin_inset CommandInset citation
  2226. LatexCommand cite
  2227. key "Leek2007"
  2228. literal "false"
  2229. \end_inset
  2230. .
  2231. Since the final batch effects are estimated from the full data, moderate
  2232. correlations between the batch effects and effects of interest are allowed,
  2233. which gives
  2234. \begin_inset Flex Glossary Term
  2235. status open
  2236. \begin_layout Plain Layout
  2237. SVA
  2238. \end_layout
  2239. \end_inset
  2240. much more freedom to estimate the true extent of the batch effects compared
  2241. to simple residual
  2242. \begin_inset Flex Glossary Term
  2243. status open
  2244. \begin_layout Plain Layout
  2245. SVD
  2246. \end_layout
  2247. \end_inset
  2248. .
  2249. Once the surrogate variables are estimated, they can be included as coefficient
  2250. s in the linear model in a similar fashion to known batch effects in order
  2251. to subtract out their effects on each feature's abundance.
  2252. \end_layout
  2253. \begin_layout Subsection
  2254. Benjamini-Hochberg + pval dist
  2255. \end_layout
  2256. \begin_layout Standard
  2257. When testing thousands of genes for differential expression or performing
  2258. thousands of statistical tests for other kinds of genomic data, the result
  2259. is thousands of p-values.
  2260. By construction, p-values have a
  2261. \begin_inset Formula $\mathrm{Uniform}(0,1)$
  2262. \end_inset
  2263. distribution under the null hypothesis.
  2264. This means that if all null hypotheses are true in a large number
  2265. \begin_inset Formula $N$
  2266. \end_inset
  2267. of tests, then for any significance threshold
  2268. \begin_inset Formula $T$
  2269. \end_inset
  2270. , approximately
  2271. \begin_inset Formula $N*T$
  2272. \end_inset
  2273. p-values will be
  2274. \begin_inset Quotes eld
  2275. \end_inset
  2276. significant
  2277. \begin_inset Quotes erd
  2278. \end_inset
  2279. at that threshold even though the null hypotheses are all true.
  2280. These are called false discoveries.
  2281. \end_layout
  2282. \begin_layout Standard
  2283. When only a fraction of null hypotheses are true, the p-value distribution
  2284. will be a mixture of a uniform component representing the null hypotheses
  2285. that are true and a non-uniform component representing the null hypotheses
  2286. that are not true.
  2287. The fraction belonging to the uniform component is referred to as
  2288. \begin_inset Formula $\pi_{0}$
  2289. \end_inset
  2290. , which ranges from 1 (all null hypotheses true) to 0 (all null hypotheses
  2291. false).
  2292. Furthermore, the non-uniform component must be biased toward zero, since
  2293. any evidence against the null hypothesis must push the p-value for a test
  2294. toward zero.
  2295. We can exploit this fact to estimate the
  2296. \begin_inset Flex Glossary Term
  2297. status open
  2298. \begin_layout Plain Layout
  2299. FDR
  2300. \end_layout
  2301. \end_inset
  2302. for any significance threshold by estimating the degree to which the density
  2303. of p-values left of that threshold exceeds what would be expected for a
  2304. uniform distribution.
  2305. In genomics, the most commonly used FDR estimation method, and the one
  2306. used in this work, is that of
  2307. \begin_inset ERT
  2308. status open
  2309. \begin_layout Plain Layout
  2310. \backslash
  2311. glsdisp{BH}{Benjamini and Hochberg}
  2312. \end_layout
  2313. \end_inset
  2314. \begin_inset CommandInset citation
  2315. LatexCommand cite
  2316. key "Benjamini1995"
  2317. literal "false"
  2318. \end_inset
  2319. .
  2320. This is a conservative method that effectively assumes
  2321. \begin_inset Formula $\pi_{0}=1$
  2322. \end_inset
  2323. unconditionally.
  2324. Hence it gives an upper bound for the FDR at any significance threshold.
  2325. \end_layout
  2326. \begin_layout Standard
  2327. \begin_inset Float figure
  2328. wide false
  2329. sideways false
  2330. status collapsed
  2331. \begin_layout Plain Layout
  2332. \align center
  2333. \begin_inset Graphics
  2334. filename graphics/Intro/med-pval-hist-colored-CROP.pdf
  2335. lyxscale 50
  2336. width 100col%
  2337. groupId colfullwidth
  2338. \end_inset
  2339. \end_layout
  2340. \begin_layout Plain Layout
  2341. \begin_inset Caption Standard
  2342. \begin_layout Plain Layout
  2343. \begin_inset Argument 1
  2344. status collapsed
  2345. \begin_layout Plain Layout
  2346. Example p-value histogram.
  2347. \end_layout
  2348. \end_inset
  2349. \begin_inset CommandInset label
  2350. LatexCommand label
  2351. name "fig:Example-pval-hist"
  2352. \end_inset
  2353. \series bold
  2354. Example p-value histogram.
  2355. \series default
  2356. The distribution of p-values from a large number of independent tests (such
  2357. as differential expression tests for each gene in the genome) is a mixture
  2358. of a uniform component representing the null hypotheses that are true (blue
  2359. shading) and a zero-biased component representing the null hypotheses that
  2360. are false (red shading).
  2361. The FDR for any column in the histogram is the fraction of that column
  2362. that is blue.
  2363. The line
  2364. \begin_inset Formula $y=\pi_{0}$
  2365. \end_inset
  2366. represents the theoretical uniform component of this p-value distribution,
  2367. while the line
  2368. \begin_inset Formula $y=1$
  2369. \end_inset
  2370. represents the uniform component when all null hypotheses are true.
  2371. Note that in real data, the true status of each hypothesis is unknown,
  2372. so only the overall shape of the distribution is known.
  2373. \end_layout
  2374. \end_inset
  2375. \end_layout
  2376. \end_inset
  2377. \end_layout
  2378. \begin_layout Subsection
  2379. Factor analysis: PCA, PCoA, MOFA
  2380. \end_layout
  2381. \begin_layout Standard
  2382. \begin_inset Flex TODO Note (inline)
  2383. status open
  2384. \begin_layout Plain Layout
  2385. Not sure if this merits a subsection here.
  2386. \end_layout
  2387. \end_inset
  2388. \end_layout
  2389. \begin_layout Itemize
  2390. Batch-corrected
  2391. \begin_inset Flex Glossary Term
  2392. status open
  2393. \begin_layout Plain Layout
  2394. PCA
  2395. \end_layout
  2396. \end_inset
  2397. is informative, but careful application is required to avoid bias
  2398. \end_layout
  2399. \begin_layout Section
  2400. Structure of the thesis
  2401. \end_layout
  2402. \begin_layout Chapter
  2403. Reproducible genome-wide epigenetic analysis of H3K4 and H3K27 methylation
  2404. in naïve and memory CD4
  2405. \begin_inset Formula $^{+}$
  2406. \end_inset
  2407. T-cell activation
  2408. \end_layout
  2409. \begin_layout Standard
  2410. \size large
  2411. Ryan C.
  2412. Thompson, Sarah A.
  2413. Lamere, Daniel R.
  2414. Salomon
  2415. \end_layout
  2416. \begin_layout Standard
  2417. \begin_inset ERT
  2418. status collapsed
  2419. \begin_layout Plain Layout
  2420. \backslash
  2421. glsresetall
  2422. \end_layout
  2423. \end_inset
  2424. \begin_inset Note Note
  2425. status collapsed
  2426. \begin_layout Plain Layout
  2427. Reintroduce all abbreviations
  2428. \end_layout
  2429. \end_inset
  2430. \end_layout
  2431. \begin_layout Standard
  2432. \begin_inset Flex TODO Note (inline)
  2433. status open
  2434. \begin_layout Plain Layout
  2435. Need better section titles throughout the entire chapter
  2436. \end_layout
  2437. \end_inset
  2438. \end_layout
  2439. \begin_layout Section
  2440. Approach
  2441. \end_layout
  2442. \begin_layout Standard
  2443. CD4
  2444. \begin_inset Formula $^{+}$
  2445. \end_inset
  2446. T-cells are central to all adaptive immune responses, as well as immune
  2447. memory
  2448. \begin_inset CommandInset citation
  2449. LatexCommand cite
  2450. key "Murphy2012"
  2451. literal "false"
  2452. \end_inset
  2453. .
  2454. After an infection is cleared, a subset of the naïve CD4
  2455. \begin_inset Formula $^{+}$
  2456. \end_inset
  2457. T-cells that responded to that infection differentiate into memory CD4
  2458. \begin_inset Formula $^{+}$
  2459. \end_inset
  2460. T-cells, which are responsible for responding to the same pathogen in the
  2461. future.
  2462. Memory CD4
  2463. \begin_inset Formula $^{+}$
  2464. \end_inset
  2465. T-cells are functionally distinct, able to respond to an infection more
  2466. quickly and without the co-stimulation required by naïve CD4
  2467. \begin_inset Formula $^{+}$
  2468. \end_inset
  2469. T-cells.
  2470. However, the molecular mechanisms underlying this functional distinction
  2471. are not well-understood.
  2472. Epigenetic regulation via histone modification is thought to play an important
  2473. role, but while many studies have looked at static snapshots of histone
  2474. methylation in T-cells, few studies have looked at the dynamics of histone
  2475. regulation after T-cell activation, nor the differences in histone methylation
  2476. between naïve and memory T-cells.
  2477. H3K4me2, H3K4me3 and H3K27me3 are three histone marks thought to be major
  2478. epigenetic regulators of gene expression.
  2479. The goal of the present study is to investigate the role of these histone
  2480. marks in CD4
  2481. \begin_inset Formula $^{+}$
  2482. \end_inset
  2483. T-cell activation kinetics and memory differentiation.
  2484. In static snapshots, H3K4me2 and H3K4me3 are often observed in the promoters
  2485. of highly transcribed genes, while H3K27me3 is more often observed in promoters
  2486. of inactive genes with little to no transcription occurring.
  2487. As a result, the two H3K4 marks have been characterized as
  2488. \begin_inset Quotes eld
  2489. \end_inset
  2490. activating
  2491. \begin_inset Quotes erd
  2492. \end_inset
  2493. marks, while H3K27me3 has been characterized as
  2494. \begin_inset Quotes eld
  2495. \end_inset
  2496. deactivating
  2497. \begin_inset Quotes erd
  2498. \end_inset
  2499. .
  2500. Despite these characterizations, the actual causal relationship between
  2501. these histone modifications and gene transcription is complex and likely
  2502. involves positive and negative feedback loops between the two.
  2503. \end_layout
  2504. \begin_layout Standard
  2505. In order to investigate the relationship between gene expression and these
  2506. histone modifications in the context of naïve and memory CD4
  2507. \begin_inset Formula $^{+}$
  2508. \end_inset
  2509. T-cell activation, a previously published data set of
  2510. \begin_inset Flex Glossary Term
  2511. status open
  2512. \begin_layout Plain Layout
  2513. RNA-seq
  2514. \end_layout
  2515. \end_inset
  2516. data and
  2517. \begin_inset Flex Glossary Term
  2518. status open
  2519. \begin_layout Plain Layout
  2520. ChIP-seq
  2521. \end_layout
  2522. \end_inset
  2523. data was re-analyzed using up-to-date methods designed to address the specific
  2524. analysis challenges posed by this data set.
  2525. The data set contains naïve and memory CD4
  2526. \begin_inset Formula $^{+}$
  2527. \end_inset
  2528. T-cell samples in a time course before and after activation.
  2529. Like the original analysis, this analysis looks at the dynamics of these
  2530. histone marks and compares them to gene expression dynamics at the same
  2531. time points during activation, as well as compares them between naïve and
  2532. memory cells, in hope of discovering evidence of new mechanistic details
  2533. in the interplay between them.
  2534. The original analysis of this data treated each gene promoter as a monolithic
  2535. unit and mostly assumed that
  2536. \begin_inset Flex Glossary Term
  2537. status open
  2538. \begin_layout Plain Layout
  2539. ChIP-seq
  2540. \end_layout
  2541. \end_inset
  2542. reads or peaks occurring anywhere within a promoter were equivalent, regardless
  2543. of where they occurred relative to the gene structure.
  2544. For an initial analysis of the data, this was a necessary simplifying assumptio
  2545. n.
  2546. The current analysis aims to relax this assumption, first by directly analyzing
  2547. \begin_inset Flex Glossary Term
  2548. status open
  2549. \begin_layout Plain Layout
  2550. ChIP-seq
  2551. \end_layout
  2552. \end_inset
  2553. peaks for differential modification, and second by taking a more granular
  2554. look at the
  2555. \begin_inset Flex Glossary Term
  2556. status open
  2557. \begin_layout Plain Layout
  2558. ChIP-seq
  2559. \end_layout
  2560. \end_inset
  2561. read coverage within promoter regions to ask whether the location of histone
  2562. modifications relative to the gene's
  2563. \begin_inset Flex Glossary Term
  2564. status open
  2565. \begin_layout Plain Layout
  2566. TSS
  2567. \end_layout
  2568. \end_inset
  2569. is an important factor, as opposed to simple proximity.
  2570. \end_layout
  2571. \begin_layout Section
  2572. Methods
  2573. \end_layout
  2574. \begin_layout Standard
  2575. A reproducible workflow was written to analyze the raw
  2576. \begin_inset Flex Glossary Term
  2577. status open
  2578. \begin_layout Plain Layout
  2579. ChIP-seq
  2580. \end_layout
  2581. \end_inset
  2582. and
  2583. \begin_inset Flex Glossary Term
  2584. status open
  2585. \begin_layout Plain Layout
  2586. RNA-seq
  2587. \end_layout
  2588. \end_inset
  2589. data from previous studies
  2590. \begin_inset CommandInset citation
  2591. LatexCommand cite
  2592. key "gh-cd4-csaw,LaMere2016,LaMere2017"
  2593. literal "true"
  2594. \end_inset
  2595. .
  2596. Briefly, this data consists of
  2597. \begin_inset Flex Glossary Term
  2598. status open
  2599. \begin_layout Plain Layout
  2600. RNA-seq
  2601. \end_layout
  2602. \end_inset
  2603. and
  2604. \begin_inset Flex Glossary Term
  2605. status open
  2606. \begin_layout Plain Layout
  2607. ChIP-seq
  2608. \end_layout
  2609. \end_inset
  2610. from CD4
  2611. \begin_inset Formula $^{+}$
  2612. \end_inset
  2613. T-cells from 4 donors.
  2614. From each donor, naïve and memory CD4
  2615. \begin_inset Formula $^{+}$
  2616. \end_inset
  2617. T-cells were isolated separately.
  2618. Then cultures of both cells were activated with CD3/CD28 beads, and samples
  2619. were taken at 4 time points: Day 0 (pre-activation), Day 1 (early activation),
  2620. Day 5 (peak activation), and Day 14 (post-activation).
  2621. For each combination of cell type and time point, RNA was isolated and
  2622. sequenced, and
  2623. \begin_inset Flex Glossary Term
  2624. status open
  2625. \begin_layout Plain Layout
  2626. ChIP-seq
  2627. \end_layout
  2628. \end_inset
  2629. was performed for each of 3 histone marks: H3K4me2, H3K4me3, and H3K27me3.
  2630. The
  2631. \begin_inset Flex Glossary Term
  2632. status open
  2633. \begin_layout Plain Layout
  2634. ChIP-seq
  2635. \end_layout
  2636. \end_inset
  2637. input DNA was also sequenced for each sample.
  2638. The result was 32 samples for each assay.
  2639. \end_layout
  2640. \begin_layout Subsection
  2641. RNA-seq differential expression analysis
  2642. \end_layout
  2643. \begin_layout Standard
  2644. \begin_inset Note Note
  2645. status collapsed
  2646. \begin_layout Plain Layout
  2647. \begin_inset Float figure
  2648. wide false
  2649. sideways false
  2650. status open
  2651. \begin_layout Plain Layout
  2652. \align center
  2653. \begin_inset Float figure
  2654. wide false
  2655. sideways false
  2656. status collapsed
  2657. \begin_layout Plain Layout
  2658. \align center
  2659. \begin_inset Graphics
  2660. filename graphics/CD4-csaw/rnaseq-compare/ensmebl-vs-entrez-star-CROP.png
  2661. lyxscale 25
  2662. width 35col%
  2663. groupId rna-comp-subfig
  2664. \end_inset
  2665. \end_layout
  2666. \begin_layout Plain Layout
  2667. \begin_inset Caption Standard
  2668. \begin_layout Plain Layout
  2669. STAR quantification, Entrez vs Ensembl gene annotation
  2670. \end_layout
  2671. \end_inset
  2672. \end_layout
  2673. \end_inset
  2674. \begin_inset space \qquad{}
  2675. \end_inset
  2676. \begin_inset Float figure
  2677. wide false
  2678. sideways false
  2679. status collapsed
  2680. \begin_layout Plain Layout
  2681. \align center
  2682. \begin_inset Graphics
  2683. filename graphics/CD4-csaw/rnaseq-compare/ensmebl-vs-entrez-shoal-CROP.png
  2684. lyxscale 25
  2685. width 35col%
  2686. groupId rna-comp-subfig
  2687. \end_inset
  2688. \end_layout
  2689. \begin_layout Plain Layout
  2690. \begin_inset Caption Standard
  2691. \begin_layout Plain Layout
  2692. Salmon+Shoal quantification, Entrez vs Ensembl gene annotation
  2693. \end_layout
  2694. \end_inset
  2695. \end_layout
  2696. \end_inset
  2697. \end_layout
  2698. \begin_layout Plain Layout
  2699. \align center
  2700. \begin_inset Float figure
  2701. wide false
  2702. sideways false
  2703. status collapsed
  2704. \begin_layout Plain Layout
  2705. \align center
  2706. \begin_inset Graphics
  2707. filename graphics/CD4-csaw/rnaseq-compare/star-vs-hisat2-CROP.png
  2708. lyxscale 25
  2709. width 35col%
  2710. groupId rna-comp-subfig
  2711. \end_inset
  2712. \end_layout
  2713. \begin_layout Plain Layout
  2714. \begin_inset Caption Standard
  2715. \begin_layout Plain Layout
  2716. STAR vs HISAT2 quantification, Ensembl gene annotation
  2717. \end_layout
  2718. \end_inset
  2719. \end_layout
  2720. \end_inset
  2721. \begin_inset space \qquad{}
  2722. \end_inset
  2723. \begin_inset Float figure
  2724. wide false
  2725. sideways false
  2726. status collapsed
  2727. \begin_layout Plain Layout
  2728. \align center
  2729. \begin_inset Graphics
  2730. filename graphics/CD4-csaw/rnaseq-compare/star-vs-salmon-CROP.png
  2731. lyxscale 25
  2732. width 35col%
  2733. groupId rna-comp-subfig
  2734. \end_inset
  2735. \end_layout
  2736. \begin_layout Plain Layout
  2737. \begin_inset Caption Standard
  2738. \begin_layout Plain Layout
  2739. Salmon vs STAR quantification, Ensembl gene annotation
  2740. \end_layout
  2741. \end_inset
  2742. \end_layout
  2743. \end_inset
  2744. \end_layout
  2745. \begin_layout Plain Layout
  2746. \align center
  2747. \begin_inset Float figure
  2748. wide false
  2749. sideways false
  2750. status collapsed
  2751. \begin_layout Plain Layout
  2752. \align center
  2753. \begin_inset Graphics
  2754. filename graphics/CD4-csaw/rnaseq-compare/salmon-vs-kallisto-CROP.png
  2755. lyxscale 25
  2756. width 35col%
  2757. groupId rna-comp-subfig
  2758. \end_inset
  2759. \end_layout
  2760. \begin_layout Plain Layout
  2761. \begin_inset Caption Standard
  2762. \begin_layout Plain Layout
  2763. Salmon vs Kallisto quantification, Ensembl gene annotation
  2764. \end_layout
  2765. \end_inset
  2766. \end_layout
  2767. \end_inset
  2768. \begin_inset space \qquad{}
  2769. \end_inset
  2770. \begin_inset Float figure
  2771. wide false
  2772. sideways false
  2773. status collapsed
  2774. \begin_layout Plain Layout
  2775. \align center
  2776. \begin_inset Graphics
  2777. filename graphics/CD4-csaw/rnaseq-compare/salmon-vs-shoal-CROP.png
  2778. lyxscale 25
  2779. width 35col%
  2780. groupId rna-comp-subfig
  2781. \end_inset
  2782. \end_layout
  2783. \begin_layout Plain Layout
  2784. \begin_inset Caption Standard
  2785. \begin_layout Plain Layout
  2786. Salmon+Shoal vs Salmon alone, Ensembl gene annotation
  2787. \end_layout
  2788. \end_inset
  2789. \end_layout
  2790. \end_inset
  2791. \end_layout
  2792. \begin_layout Plain Layout
  2793. \begin_inset Caption Standard
  2794. \begin_layout Plain Layout
  2795. \begin_inset CommandInset label
  2796. LatexCommand label
  2797. name "fig:RNA-norm-comp"
  2798. \end_inset
  2799. RNA-seq comparisons
  2800. \end_layout
  2801. \end_inset
  2802. \end_layout
  2803. \end_inset
  2804. \end_layout
  2805. \end_inset
  2806. \end_layout
  2807. \begin_layout Standard
  2808. Sequence reads were retrieved from the
  2809. \begin_inset Flex Glossary Term
  2810. status open
  2811. \begin_layout Plain Layout
  2812. SRA
  2813. \end_layout
  2814. \end_inset
  2815. \begin_inset CommandInset citation
  2816. LatexCommand cite
  2817. key "Leinonen2011"
  2818. literal "false"
  2819. \end_inset
  2820. .
  2821. Five different alignment and quantification methods were tested for the
  2822. \begin_inset Flex Glossary Term
  2823. status open
  2824. \begin_layout Plain Layout
  2825. RNA-seq
  2826. \end_layout
  2827. \end_inset
  2828. data
  2829. \begin_inset CommandInset citation
  2830. LatexCommand cite
  2831. key "Dobin2012,Kim2019,Liao2014,Pimentel2016,Patro2017,gh-shoal,gh-hg38-ref"
  2832. literal "false"
  2833. \end_inset
  2834. .
  2835. Each quantification was tested with both Ensembl transcripts and GENCODE
  2836. known gene annotations
  2837. \begin_inset CommandInset citation
  2838. LatexCommand cite
  2839. key "Zerbino2018,Harrow2012"
  2840. literal "false"
  2841. \end_inset
  2842. .
  2843. Comparisons of downstream results from each combination of quantification
  2844. method and reference revealed that all quantifications gave broadly similar
  2845. results for most genes, with non being obviously superior.
  2846. Salmon quantification with regularization by shoal with the Ensembl annotation
  2847. was chosen as the method theoretically most likely to partially mitigate
  2848. some of the batch effect in the data
  2849. \begin_inset CommandInset citation
  2850. LatexCommand cite
  2851. key "gh-shoal,Patro2017"
  2852. literal "false"
  2853. \end_inset
  2854. .
  2855. \end_layout
  2856. \begin_layout Standard
  2857. Due to an error in sample preparation, the RNA from the samples for days
  2858. 0 and 5 were sequenced using a different kit than those for days 1 and
  2859. 14.
  2860. This induced a substantial batch effect in the data due to differences
  2861. in sequencing biases between the two kits, and this batch effect is unfortunate
  2862. ly confounded with the time point variable (Figure
  2863. \begin_inset CommandInset ref
  2864. LatexCommand ref
  2865. reference "fig:RNA-PCA-no-batchsub"
  2866. plural "false"
  2867. caps "false"
  2868. noprefix "false"
  2869. \end_inset
  2870. ).
  2871. To do the best possible analysis with this data, this batch effect was
  2872. subtracted out from the data using ComBat
  2873. \begin_inset CommandInset citation
  2874. LatexCommand cite
  2875. key "Johnson2007"
  2876. literal "false"
  2877. \end_inset
  2878. , ignoring the time point variable due to the confounding with the batch
  2879. variable.
  2880. The result is a marked improvement, but the unavoidable confounding with
  2881. time point means that certain real patterns of gene expression will be
  2882. indistinguishable from the batch effect and subtracted out as a result.
  2883. Specifically, any
  2884. \begin_inset Quotes eld
  2885. \end_inset
  2886. zig-zag
  2887. \begin_inset Quotes erd
  2888. \end_inset
  2889. pattern, such as a gene whose expression goes up on day 1, down on day
  2890. 5, and back up again on day 14, will be attenuated or eliminated entirely.
  2891. In the context of a T-cell activation time course, it is unlikely that
  2892. many genes of interest will follow such an expression pattern, so this
  2893. loss was deemed an acceptable cost for correcting the batch effect.
  2894. \end_layout
  2895. \begin_layout Standard
  2896. \begin_inset Float figure
  2897. wide false
  2898. sideways false
  2899. status collapsed
  2900. \begin_layout Plain Layout
  2901. \align center
  2902. \begin_inset Float figure
  2903. wide false
  2904. sideways false
  2905. status open
  2906. \begin_layout Plain Layout
  2907. \align center
  2908. \begin_inset Graphics
  2909. filename graphics/CD4-csaw/RNA-seq/PCA-no-batchsub-CROP.png
  2910. lyxscale 25
  2911. width 75col%
  2912. groupId rna-pca-subfig
  2913. \end_inset
  2914. \end_layout
  2915. \begin_layout Plain Layout
  2916. \begin_inset Caption Standard
  2917. \begin_layout Plain Layout
  2918. \begin_inset CommandInset label
  2919. LatexCommand label
  2920. name "fig:RNA-PCA-no-batchsub"
  2921. \end_inset
  2922. Before batch correction
  2923. \end_layout
  2924. \end_inset
  2925. \end_layout
  2926. \end_inset
  2927. \end_layout
  2928. \begin_layout Plain Layout
  2929. \align center
  2930. \begin_inset Float figure
  2931. wide false
  2932. sideways false
  2933. status open
  2934. \begin_layout Plain Layout
  2935. \align center
  2936. \begin_inset Graphics
  2937. filename graphics/CD4-csaw/RNA-seq/PCA-combat-batchsub-CROP.png
  2938. lyxscale 25
  2939. width 75col%
  2940. groupId rna-pca-subfig
  2941. \end_inset
  2942. \end_layout
  2943. \begin_layout Plain Layout
  2944. \begin_inset Caption Standard
  2945. \begin_layout Plain Layout
  2946. \begin_inset CommandInset label
  2947. LatexCommand label
  2948. name "fig:RNA-PCA-ComBat-batchsub"
  2949. \end_inset
  2950. After batch correction with ComBat
  2951. \end_layout
  2952. \end_inset
  2953. \end_layout
  2954. \end_inset
  2955. \end_layout
  2956. \begin_layout Plain Layout
  2957. \begin_inset Caption Standard
  2958. \begin_layout Plain Layout
  2959. \begin_inset Argument 1
  2960. status collapsed
  2961. \begin_layout Plain Layout
  2962. PCoA plots of RNA-seq data showing effect of batch correction.
  2963. \end_layout
  2964. \end_inset
  2965. \begin_inset CommandInset label
  2966. LatexCommand label
  2967. name "fig:RNA-PCA"
  2968. \end_inset
  2969. \series bold
  2970. PCoA plots of RNA-seq data showing effect of batch correction.
  2971. \series default
  2972. The uncorrected data (a) shows a clear separation between samples from the
  2973. two batches (red and blue) dominating the first principal coordinate.
  2974. After correction with ComBat (b), the two batches now have approximately
  2975. the same center, and the first two principal coordinates both show separation
  2976. between experimental conditions rather than batches.
  2977. (Note that time points are shown in hours rather than days in these plots.)
  2978. \end_layout
  2979. \end_inset
  2980. \end_layout
  2981. \end_inset
  2982. \end_layout
  2983. \begin_layout Standard
  2984. However, removing the systematic component of the batch effect still leaves
  2985. the noise component.
  2986. The gene quantifications from the first batch are substantially noisier
  2987. than those in the second batch.
  2988. This analysis corrected for this by using
  2989. \begin_inset Flex Code
  2990. status open
  2991. \begin_layout Plain Layout
  2992. limma
  2993. \end_layout
  2994. \end_inset
  2995. 's sample weighting method to assign lower weights to the noisy samples
  2996. of batch 1 (Figure
  2997. \begin_inset CommandInset ref
  2998. LatexCommand ref
  2999. reference "fig:RNA-seq-weights-vs-covars"
  3000. plural "false"
  3001. caps "false"
  3002. noprefix "false"
  3003. \end_inset
  3004. )
  3005. \begin_inset CommandInset citation
  3006. LatexCommand cite
  3007. key "Ritchie2006,Liu2015"
  3008. literal "false"
  3009. \end_inset
  3010. .
  3011. The resulting analysis gives an accurate assessment of statistical significance
  3012. for all comparisons, which unfortunately means a loss of statistical power
  3013. for comparisons involving samples in batch 1.
  3014. \end_layout
  3015. \begin_layout Standard
  3016. In any case, the
  3017. \begin_inset Flex Glossary Term
  3018. status open
  3019. \begin_layout Plain Layout
  3020. RNA-seq
  3021. \end_layout
  3022. \end_inset
  3023. counts were first normalized using
  3024. \begin_inset Flex Glossary Term
  3025. status open
  3026. \begin_layout Plain Layout
  3027. TMM
  3028. \end_layout
  3029. \end_inset
  3030. \begin_inset CommandInset citation
  3031. LatexCommand cite
  3032. key "Robinson2010"
  3033. literal "false"
  3034. \end_inset
  3035. , converted to normalized
  3036. \begin_inset Flex Glossary Term
  3037. status open
  3038. \begin_layout Plain Layout
  3039. logCPM
  3040. \end_layout
  3041. \end_inset
  3042. with quality weights using
  3043. \begin_inset Flex Code
  3044. status open
  3045. \begin_layout Plain Layout
  3046. voomWithQualityWeights
  3047. \end_layout
  3048. \end_inset
  3049. \begin_inset CommandInset citation
  3050. LatexCommand cite
  3051. key "Law2013,Liu2015"
  3052. literal "false"
  3053. \end_inset
  3054. , and batch-corrected at this point using ComBat.
  3055. A linear model was fit to the batch-corrected, quality-weighted data for
  3056. each gene using
  3057. \begin_inset Flex Code
  3058. status open
  3059. \begin_layout Plain Layout
  3060. limma
  3061. \end_layout
  3062. \end_inset
  3063. , and each gene was tested for differential expression using
  3064. \begin_inset Flex Code
  3065. status open
  3066. \begin_layout Plain Layout
  3067. limma
  3068. \end_layout
  3069. \end_inset
  3070. 's empirical Bayes moderated
  3071. \begin_inset Formula $t$
  3072. \end_inset
  3073. -test
  3074. \begin_inset CommandInset citation
  3075. LatexCommand cite
  3076. key "Smyth2005,Law2013,Phipson2013"
  3077. literal "false"
  3078. \end_inset
  3079. .
  3080. P-values were corrected for multiple testing using the
  3081. \begin_inset Flex Glossary Term
  3082. status open
  3083. \begin_layout Plain Layout
  3084. BH
  3085. \end_layout
  3086. \end_inset
  3087. procedure for
  3088. \begin_inset Flex Glossary Term
  3089. status open
  3090. \begin_layout Plain Layout
  3091. FDR
  3092. \end_layout
  3093. \end_inset
  3094. control
  3095. \begin_inset CommandInset citation
  3096. LatexCommand cite
  3097. key "Benjamini1995"
  3098. literal "false"
  3099. \end_inset
  3100. .
  3101. \end_layout
  3102. \begin_layout Standard
  3103. \begin_inset Float figure
  3104. wide false
  3105. sideways false
  3106. status open
  3107. \begin_layout Plain Layout
  3108. \align center
  3109. \begin_inset Graphics
  3110. filename graphics/CD4-csaw/RNA-seq/weights-vs-covars-nobcv-CROP.png
  3111. lyxscale 25
  3112. width 100col%
  3113. groupId colwidth-raster
  3114. \end_inset
  3115. \end_layout
  3116. \begin_layout Plain Layout
  3117. \begin_inset Caption Standard
  3118. \begin_layout Plain Layout
  3119. \begin_inset Argument 1
  3120. status collapsed
  3121. \begin_layout Plain Layout
  3122. RNA-seq sample weights, grouped by experimental and technical covariates.
  3123. \end_layout
  3124. \end_inset
  3125. \begin_inset CommandInset label
  3126. LatexCommand label
  3127. name "fig:RNA-seq-weights-vs-covars"
  3128. \end_inset
  3129. \series bold
  3130. RNA-seq sample weights, grouped by experimental and technical covariates.
  3131. \series default
  3132. Inverse variance weights were estimated for each sample using
  3133. \begin_inset Flex Code
  3134. status open
  3135. \begin_layout Plain Layout
  3136. limma
  3137. \end_layout
  3138. \end_inset
  3139. 's
  3140. \begin_inset Flex Code
  3141. status open
  3142. \begin_layout Plain Layout
  3143. arrayWeights
  3144. \end_layout
  3145. \end_inset
  3146. function (part of
  3147. \begin_inset Flex Code
  3148. status open
  3149. \begin_layout Plain Layout
  3150. voomWithQualityWeights
  3151. \end_layout
  3152. \end_inset
  3153. ).
  3154. The samples were grouped by each known covariate and the distribution of
  3155. weights was plotted for each group.
  3156. \end_layout
  3157. \end_inset
  3158. \end_layout
  3159. \end_inset
  3160. \end_layout
  3161. \begin_layout Subsection
  3162. ChIP-seq analysis
  3163. \end_layout
  3164. \begin_layout Standard
  3165. \begin_inset Flex TODO Note (inline)
  3166. status open
  3167. \begin_layout Plain Layout
  3168. Be consistent about use of
  3169. \begin_inset Quotes eld
  3170. \end_inset
  3171. differential binding
  3172. \begin_inset Quotes erd
  3173. \end_inset
  3174. vs
  3175. \begin_inset Quotes eld
  3176. \end_inset
  3177. differential modification
  3178. \begin_inset Quotes erd
  3179. \end_inset
  3180. throughout this chapter.
  3181. The latter is usually preferred.
  3182. \end_layout
  3183. \end_inset
  3184. \end_layout
  3185. \begin_layout Standard
  3186. Sequence reads were retrieved from
  3187. \begin_inset Flex Glossary Term
  3188. status open
  3189. \begin_layout Plain Layout
  3190. SRA
  3191. \end_layout
  3192. \end_inset
  3193. \begin_inset CommandInset citation
  3194. LatexCommand cite
  3195. key "Leinonen2011"
  3196. literal "false"
  3197. \end_inset
  3198. .
  3199. \begin_inset Flex Glossary Term (Capital)
  3200. status open
  3201. \begin_layout Plain Layout
  3202. ChIP-seq
  3203. \end_layout
  3204. \end_inset
  3205. (and input) reads were aligned to the
  3206. \begin_inset Flex Glossary Term
  3207. status open
  3208. \begin_layout Plain Layout
  3209. GRCh38
  3210. \end_layout
  3211. \end_inset
  3212. genome assembly using Bowtie 2
  3213. \begin_inset CommandInset citation
  3214. LatexCommand cite
  3215. key "Langmead2012,Schneider2017,gh-hg38-ref"
  3216. literal "false"
  3217. \end_inset
  3218. .
  3219. Artifact regions were annotated using a custom implementation of the
  3220. \begin_inset Flex Code
  3221. status open
  3222. \begin_layout Plain Layout
  3223. GreyListChIP
  3224. \end_layout
  3225. \end_inset
  3226. algorithm, and these
  3227. \begin_inset Quotes eld
  3228. \end_inset
  3229. greylists
  3230. \begin_inset Quotes erd
  3231. \end_inset
  3232. were merged with the published
  3233. \begin_inset Flex Glossary Term
  3234. status open
  3235. \begin_layout Plain Layout
  3236. ENCODE
  3237. \end_layout
  3238. \end_inset
  3239. blacklists
  3240. \begin_inset CommandInset citation
  3241. LatexCommand cite
  3242. key "greylistchip,Dunham2012,Amemiya2019,gh-cd4-csaw"
  3243. literal "false"
  3244. \end_inset
  3245. .
  3246. Any read or called peak overlapping one of these regions was regarded as
  3247. artifactual and excluded from downstream analyses.
  3248. Figure
  3249. \begin_inset CommandInset ref
  3250. LatexCommand ref
  3251. reference "fig:CCF-master"
  3252. plural "false"
  3253. caps "false"
  3254. noprefix "false"
  3255. \end_inset
  3256. shows the improvement after blacklisting in the strand cross-correlation
  3257. plots, a common quality control plot for
  3258. \begin_inset Flex Glossary Term
  3259. status open
  3260. \begin_layout Plain Layout
  3261. ChIP-seq
  3262. \end_layout
  3263. \end_inset
  3264. data
  3265. \begin_inset CommandInset citation
  3266. LatexCommand cite
  3267. key "Kharchenko2008,Lun2015a"
  3268. literal "false"
  3269. \end_inset
  3270. .
  3271. Peaks were called using
  3272. \begin_inset Flex Code
  3273. status open
  3274. \begin_layout Plain Layout
  3275. epic
  3276. \end_layout
  3277. \end_inset
  3278. , an implementation of the
  3279. \begin_inset Flex Glossary Term
  3280. status open
  3281. \begin_layout Plain Layout
  3282. SICER
  3283. \end_layout
  3284. \end_inset
  3285. algorithm
  3286. \begin_inset CommandInset citation
  3287. LatexCommand cite
  3288. key "Zang2009,gh-epic"
  3289. literal "false"
  3290. \end_inset
  3291. .
  3292. Peaks were also called separately using
  3293. \begin_inset Flex Glossary Term
  3294. status open
  3295. \begin_layout Plain Layout
  3296. MACS
  3297. \end_layout
  3298. \end_inset
  3299. , but
  3300. \begin_inset Flex Glossary Term
  3301. status open
  3302. \begin_layout Plain Layout
  3303. MACS
  3304. \end_layout
  3305. \end_inset
  3306. was determined to be a poor fit for the data, and these peak calls are
  3307. not used in any further analyses
  3308. \begin_inset CommandInset citation
  3309. LatexCommand cite
  3310. key "Zhang2008"
  3311. literal "false"
  3312. \end_inset
  3313. .
  3314. Consensus peaks were determined by applying the
  3315. \begin_inset Flex Glossary Term
  3316. status open
  3317. \begin_layout Plain Layout
  3318. IDR
  3319. \end_layout
  3320. \end_inset
  3321. framework
  3322. \begin_inset CommandInset citation
  3323. LatexCommand cite
  3324. key "Li2006,gh-idr"
  3325. literal "false"
  3326. \end_inset
  3327. to find peaks consistently called in the same locations across all 4 donors.
  3328. \end_layout
  3329. \begin_layout Standard
  3330. \begin_inset Float figure
  3331. wide false
  3332. sideways false
  3333. status collapsed
  3334. \begin_layout Plain Layout
  3335. \align center
  3336. \begin_inset Float figure
  3337. wide false
  3338. sideways false
  3339. status open
  3340. \begin_layout Plain Layout
  3341. \align center
  3342. \begin_inset Graphics
  3343. filename graphics/CD4-csaw/csaw/CCF-plots-noBL-PAGE2-CROP.pdf
  3344. lyxscale 75
  3345. height 35theight%
  3346. groupId ccf-subfig
  3347. \end_inset
  3348. \end_layout
  3349. \begin_layout Plain Layout
  3350. \begin_inset Caption Standard
  3351. \begin_layout Plain Layout
  3352. \series bold
  3353. \begin_inset CommandInset label
  3354. LatexCommand label
  3355. name "fig:CCF-without-blacklist"
  3356. \end_inset
  3357. Cross-correlation plots without removing blacklisted reads.
  3358. \series default
  3359. Without blacklisting, many artifactual peaks are visible in the cross-correlatio
  3360. ns of the ChIP-seq samples, and the peak at the true fragment size (147
  3361. \begin_inset space ~
  3362. \end_inset
  3363. bp) is frequently overshadowed by the artifactual peak at the read length
  3364. (100
  3365. \begin_inset space ~
  3366. \end_inset
  3367. bp).
  3368. \end_layout
  3369. \end_inset
  3370. \end_layout
  3371. \end_inset
  3372. \end_layout
  3373. \begin_layout Plain Layout
  3374. \align center
  3375. \begin_inset Float figure
  3376. wide false
  3377. sideways false
  3378. status open
  3379. \begin_layout Plain Layout
  3380. \align center
  3381. \begin_inset Graphics
  3382. filename graphics/CD4-csaw/csaw/CCF-plots-PAGE2-CROP.pdf
  3383. lyxscale 75
  3384. height 35theight%
  3385. groupId ccf-subfig
  3386. \end_inset
  3387. \end_layout
  3388. \begin_layout Plain Layout
  3389. \begin_inset Caption Standard
  3390. \begin_layout Plain Layout
  3391. \series bold
  3392. \begin_inset CommandInset label
  3393. LatexCommand label
  3394. name "fig:CCF-with-blacklist"
  3395. \end_inset
  3396. Cross-correlation plots with blacklisted reads removed.
  3397. \series default
  3398. After blacklisting, most ChIP-seq samples have clean-looking periodic cross-cor
  3399. relation plots, with the largest peak around 147
  3400. \begin_inset space ~
  3401. \end_inset
  3402. bp, the expected size for a fragment of DNA from a single nucleosome, and
  3403. little to no peak at the read length, 100
  3404. \begin_inset space ~
  3405. \end_inset
  3406. bp.
  3407. \end_layout
  3408. \end_inset
  3409. \end_layout
  3410. \end_inset
  3411. \end_layout
  3412. \begin_layout Plain Layout
  3413. \begin_inset Flex TODO Note (inline)
  3414. status open
  3415. \begin_layout Plain Layout
  3416. Figure font too small
  3417. \end_layout
  3418. \end_inset
  3419. \end_layout
  3420. \begin_layout Plain Layout
  3421. \begin_inset Caption Standard
  3422. \begin_layout Plain Layout
  3423. \begin_inset Argument 1
  3424. status collapsed
  3425. \begin_layout Plain Layout
  3426. Strand cross-correlation plots for ChIP-seq data, before and after blacklisting.
  3427. \end_layout
  3428. \end_inset
  3429. \begin_inset CommandInset label
  3430. LatexCommand label
  3431. name "fig:CCF-master"
  3432. \end_inset
  3433. \series bold
  3434. Strand cross-correlation plots for ChIP-seq data, before and after blacklisting.
  3435. \series default
  3436. The number of reads starting at each position in the genome was counted
  3437. separately for the plus and minus strands, and then the correlation coefficient
  3438. between the read start counts for both strands (cross-correlation) was
  3439. computed after shifting the plus strand counts forward by a specified interval
  3440. (the delay).
  3441. This was repeated for every delay value from 0 to 1000, and the cross-correlati
  3442. on values were plotted as a function of the delay.
  3443. In good quality samples, cross-correlation is maximized when the delay
  3444. equals the fragment size; in poor quality samples, cross-correlation is
  3445. often maximized when the delay equals the read length, an artifactual peak
  3446. whose cause is not fully understood.
  3447. \end_layout
  3448. \end_inset
  3449. \end_layout
  3450. \end_inset
  3451. \end_layout
  3452. \begin_layout Standard
  3453. Promoters were defined by computing the distance from each annotated
  3454. \begin_inset Flex Glossary Term
  3455. status open
  3456. \begin_layout Plain Layout
  3457. TSS
  3458. \end_layout
  3459. \end_inset
  3460. to the nearest called peak and examining the distribution of distances,
  3461. observing that peaks for each histone mark were enriched within a certain
  3462. distance of the
  3463. \begin_inset Flex Glossary Term
  3464. status open
  3465. \begin_layout Plain Layout
  3466. TSS
  3467. \end_layout
  3468. \end_inset
  3469. .
  3470. (Note: this analysis was performed using the original peak calls and expression
  3471. values from
  3472. \begin_inset Flex Glossary Term
  3473. status open
  3474. \begin_layout Plain Layout
  3475. GEO
  3476. \end_layout
  3477. \end_inset
  3478. \begin_inset CommandInset citation
  3479. LatexCommand cite
  3480. key "LaMere2016"
  3481. literal "false"
  3482. \end_inset
  3483. .) For H3K4me2 and H3K4me3, this distance was about 1
  3484. \begin_inset space ~
  3485. \end_inset
  3486. kb, while for H3K27me3 it was 2.5
  3487. \begin_inset space ~
  3488. \end_inset
  3489. kb.
  3490. These distances were used as an
  3491. \begin_inset Quotes eld
  3492. \end_inset
  3493. effective promoter radius
  3494. \begin_inset Quotes erd
  3495. \end_inset
  3496. for each mark.
  3497. The promoter region for each gene was defined as the region of the genome
  3498. within this distance upstream or downstream of the gene's annotated
  3499. \begin_inset Flex Glossary Term
  3500. status open
  3501. \begin_layout Plain Layout
  3502. TSS
  3503. \end_layout
  3504. \end_inset
  3505. .
  3506. For genes with multiple annotated
  3507. \begin_inset Flex Glossary Term (pl)
  3508. status open
  3509. \begin_layout Plain Layout
  3510. TSS
  3511. \end_layout
  3512. \end_inset
  3513. , a promoter region was defined for each
  3514. \begin_inset Flex Glossary Term
  3515. status open
  3516. \begin_layout Plain Layout
  3517. TSS
  3518. \end_layout
  3519. \end_inset
  3520. individually, and any promoters that overlapped (due to multiple
  3521. \begin_inset Flex Glossary Term (pl)
  3522. status open
  3523. \begin_layout Plain Layout
  3524. TSS
  3525. \end_layout
  3526. \end_inset
  3527. being closer than 2 times the radius) were merged into one large promoter.
  3528. Thus, some genes had multiple promoters defined, which were each analyzed
  3529. separately for differential modification.
  3530. \end_layout
  3531. \begin_layout Standard
  3532. Reads in promoters, peaks, and sliding windows across the genome were counted
  3533. and normalized using
  3534. \begin_inset Flex Code
  3535. status open
  3536. \begin_layout Plain Layout
  3537. csaw
  3538. \end_layout
  3539. \end_inset
  3540. and analyzed for differential modification using
  3541. \begin_inset Flex Code
  3542. status open
  3543. \begin_layout Plain Layout
  3544. edgeR
  3545. \end_layout
  3546. \end_inset
  3547. \begin_inset CommandInset citation
  3548. LatexCommand cite
  3549. key "Lun2014,Lun2015a,Lund2012,Phipson2016"
  3550. literal "false"
  3551. \end_inset
  3552. .
  3553. Unobserved confounding factors in the
  3554. \begin_inset Flex Glossary Term
  3555. status open
  3556. \begin_layout Plain Layout
  3557. ChIP-seq
  3558. \end_layout
  3559. \end_inset
  3560. data were corrected using
  3561. \begin_inset Flex Glossary Term
  3562. status open
  3563. \begin_layout Plain Layout
  3564. SVA
  3565. \end_layout
  3566. \end_inset
  3567. \begin_inset CommandInset citation
  3568. LatexCommand cite
  3569. key "Leek2007,Leek2014"
  3570. literal "false"
  3571. \end_inset
  3572. .
  3573. Principal coordinate plots of the promoter count data for each histone
  3574. mark before and after subtracting surrogate variable effects are shown
  3575. in Figure
  3576. \begin_inset CommandInset ref
  3577. LatexCommand ref
  3578. reference "fig:PCoA-ChIP"
  3579. plural "false"
  3580. caps "false"
  3581. noprefix "false"
  3582. \end_inset
  3583. .
  3584. \end_layout
  3585. \begin_layout Standard
  3586. \begin_inset Float figure
  3587. wide false
  3588. sideways false
  3589. status collapsed
  3590. \begin_layout Plain Layout
  3591. \begin_inset Float figure
  3592. wide false
  3593. sideways false
  3594. status open
  3595. \begin_layout Plain Layout
  3596. \align center
  3597. \begin_inset Graphics
  3598. filename graphics/CD4-csaw/ChIP-seq/H3K4me2-PCA-raw-CROP.png
  3599. lyxscale 25
  3600. width 45col%
  3601. groupId pcoa-subfig
  3602. \end_inset
  3603. \end_layout
  3604. \begin_layout Plain Layout
  3605. \begin_inset Caption Standard
  3606. \begin_layout Plain Layout
  3607. \series bold
  3608. \begin_inset CommandInset label
  3609. LatexCommand label
  3610. name "fig:PCoA-H3K4me2-bad"
  3611. \end_inset
  3612. H3K4me2, no correction
  3613. \end_layout
  3614. \end_inset
  3615. \end_layout
  3616. \end_inset
  3617. \begin_inset space \hfill{}
  3618. \end_inset
  3619. \begin_inset Float figure
  3620. wide false
  3621. sideways false
  3622. status open
  3623. \begin_layout Plain Layout
  3624. \align center
  3625. \begin_inset Graphics
  3626. filename graphics/CD4-csaw/ChIP-seq/H3K4me2-PCA-SVsub-CROP.png
  3627. lyxscale 25
  3628. width 45col%
  3629. groupId pcoa-subfig
  3630. \end_inset
  3631. \end_layout
  3632. \begin_layout Plain Layout
  3633. \begin_inset Caption Standard
  3634. \begin_layout Plain Layout
  3635. \series bold
  3636. \begin_inset CommandInset label
  3637. LatexCommand label
  3638. name "fig:PCoA-H3K4me2-good"
  3639. \end_inset
  3640. H3K4me2, SVs subtracted
  3641. \end_layout
  3642. \end_inset
  3643. \end_layout
  3644. \end_inset
  3645. \end_layout
  3646. \begin_layout Plain Layout
  3647. \begin_inset Float figure
  3648. wide false
  3649. sideways false
  3650. status collapsed
  3651. \begin_layout Plain Layout
  3652. \align center
  3653. \begin_inset Graphics
  3654. filename graphics/CD4-csaw/ChIP-seq/H3K4me3-PCA-raw-CROP.png
  3655. lyxscale 25
  3656. width 45col%
  3657. groupId pcoa-subfig
  3658. \end_inset
  3659. \end_layout
  3660. \begin_layout Plain Layout
  3661. \begin_inset Caption Standard
  3662. \begin_layout Plain Layout
  3663. \series bold
  3664. \begin_inset CommandInset label
  3665. LatexCommand label
  3666. name "fig:PCoA-H3K4me3-bad"
  3667. \end_inset
  3668. H3K4me3, no correction
  3669. \end_layout
  3670. \end_inset
  3671. \end_layout
  3672. \end_inset
  3673. \begin_inset space \hfill{}
  3674. \end_inset
  3675. \begin_inset Float figure
  3676. wide false
  3677. sideways false
  3678. status collapsed
  3679. \begin_layout Plain Layout
  3680. \align center
  3681. \begin_inset Graphics
  3682. filename graphics/CD4-csaw/ChIP-seq/H3K4me3-PCA-SVsub-CROP.png
  3683. lyxscale 25
  3684. width 45col%
  3685. groupId pcoa-subfig
  3686. \end_inset
  3687. \end_layout
  3688. \begin_layout Plain Layout
  3689. \begin_inset Caption Standard
  3690. \begin_layout Plain Layout
  3691. \series bold
  3692. \begin_inset CommandInset label
  3693. LatexCommand label
  3694. name "fig:PCoA-H3K4me3-good"
  3695. \end_inset
  3696. H3K4me3, SVs subtracted
  3697. \end_layout
  3698. \end_inset
  3699. \end_layout
  3700. \end_inset
  3701. \end_layout
  3702. \begin_layout Plain Layout
  3703. \begin_inset Float figure
  3704. wide false
  3705. sideways false
  3706. status collapsed
  3707. \begin_layout Plain Layout
  3708. \align center
  3709. \begin_inset Graphics
  3710. filename graphics/CD4-csaw/ChIP-seq/H3K27me3-PCA-raw-CROP.png
  3711. lyxscale 25
  3712. width 45col%
  3713. groupId pcoa-subfig
  3714. \end_inset
  3715. \end_layout
  3716. \begin_layout Plain Layout
  3717. \begin_inset Caption Standard
  3718. \begin_layout Plain Layout
  3719. \series bold
  3720. \begin_inset CommandInset label
  3721. LatexCommand label
  3722. name "fig:PCoA-H3K27me3-bad"
  3723. \end_inset
  3724. H3K27me3, no correction
  3725. \end_layout
  3726. \end_inset
  3727. \end_layout
  3728. \end_inset
  3729. \begin_inset space \hfill{}
  3730. \end_inset
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  3732. wide false
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  3735. \begin_layout Plain Layout
  3736. \align center
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  3738. filename graphics/CD4-csaw/ChIP-seq/H3K27me3-PCA-SVsub-CROP.png
  3739. lyxscale 25
  3740. width 45col%
  3741. groupId pcoa-subfig
  3742. \end_inset
  3743. \end_layout
  3744. \begin_layout Plain Layout
  3745. \begin_inset Caption Standard
  3746. \begin_layout Plain Layout
  3747. \series bold
  3748. \begin_inset CommandInset label
  3749. LatexCommand label
  3750. name "fig:PCoA-H3K27me3-good"
  3751. \end_inset
  3752. H3K27me3, SVs subtracted
  3753. \end_layout
  3754. \end_inset
  3755. \end_layout
  3756. \end_inset
  3757. \end_layout
  3758. \begin_layout Plain Layout
  3759. \begin_inset Flex TODO Note (inline)
  3760. status collapsed
  3761. \begin_layout Plain Layout
  3762. Figure font too small
  3763. \end_layout
  3764. \end_inset
  3765. \end_layout
  3766. \begin_layout Plain Layout
  3767. \begin_inset Caption Standard
  3768. \begin_layout Plain Layout
  3769. \begin_inset Argument 1
  3770. status collapsed
  3771. \begin_layout Plain Layout
  3772. PCoA plots of ChIP-seq sliding window data, before and after subtracting
  3773. surrogate variables.
  3774. \end_layout
  3775. \end_inset
  3776. \begin_inset CommandInset label
  3777. LatexCommand label
  3778. name "fig:PCoA-ChIP"
  3779. \end_inset
  3780. \series bold
  3781. PCoA plots of ChIP-seq sliding window data, before and after subtracting
  3782. surrogate variables (SVs).
  3783. \series default
  3784. For each histone mark, a PCoA plot of the first 2 principal coordinates
  3785. was created before and after subtraction of SV effects.
  3786. Time points are shown by color and cell type by shape, and samples from
  3787. the same time point and cell type are enclosed in a shaded area to aid
  3788. in visial recognition (this shaded area has no meaning on the plot).
  3789. Samples of the same cell type from the same donor are connected with a
  3790. line in time point order, showing the
  3791. \begin_inset Quotes eld
  3792. \end_inset
  3793. trajectory
  3794. \begin_inset Quotes erd
  3795. \end_inset
  3796. of each donor's samples over time.
  3797. \end_layout
  3798. \end_inset
  3799. \end_layout
  3800. \end_inset
  3801. \end_layout
  3802. \begin_layout Standard
  3803. To investigate whether the location of a peak within the promoter region
  3804. was important,
  3805. \begin_inset Quotes eld
  3806. \end_inset
  3807. relative coverage profiles
  3808. \begin_inset Quotes erd
  3809. \end_inset
  3810. were generated.
  3811. First, 500-bp sliding windows were tiled around each annotated
  3812. \begin_inset Flex Glossary Term
  3813. status open
  3814. \begin_layout Plain Layout
  3815. TSS
  3816. \end_layout
  3817. \end_inset
  3818. : one window centered on the
  3819. \begin_inset Flex Glossary Term
  3820. status open
  3821. \begin_layout Plain Layout
  3822. TSS
  3823. \end_layout
  3824. \end_inset
  3825. itself, and 10 windows each upstream and downstream, thus covering a 10.5-kb
  3826. region centered on the
  3827. \begin_inset Flex Glossary Term
  3828. status open
  3829. \begin_layout Plain Layout
  3830. TSS
  3831. \end_layout
  3832. \end_inset
  3833. with 21 windows.
  3834. Reads in each window for each
  3835. \begin_inset Flex Glossary Term
  3836. status open
  3837. \begin_layout Plain Layout
  3838. TSS
  3839. \end_layout
  3840. \end_inset
  3841. were counted in each sample, and the counts were normalized and converted
  3842. to
  3843. \begin_inset Flex Glossary Term
  3844. status open
  3845. \begin_layout Plain Layout
  3846. logCPM
  3847. \end_layout
  3848. \end_inset
  3849. as in the differential modification analysis.
  3850. Then, the
  3851. \begin_inset Flex Glossary Term
  3852. status open
  3853. \begin_layout Plain Layout
  3854. logCPM
  3855. \end_layout
  3856. \end_inset
  3857. values within each promoter were normalized to an average of zero, such
  3858. that each window's normalized abundance now represents the relative read
  3859. depth of that window compared to all other windows in the same promoter.
  3860. The normalized abundance values for each window in a promoter are collectively
  3861. referred to as that promoter's
  3862. \begin_inset Quotes eld
  3863. \end_inset
  3864. relative coverage profile
  3865. \begin_inset Quotes erd
  3866. \end_inset
  3867. .
  3868. \end_layout
  3869. \begin_layout Subsection
  3870. MOFA analysis of cross-dataset variation patterns
  3871. \end_layout
  3872. \begin_layout Standard
  3873. \begin_inset Flex Glossary Term
  3874. status open
  3875. \begin_layout Plain Layout
  3876. MOFA
  3877. \end_layout
  3878. \end_inset
  3879. was run on all the
  3880. \begin_inset Flex Glossary Term
  3881. status open
  3882. \begin_layout Plain Layout
  3883. ChIP-seq
  3884. \end_layout
  3885. \end_inset
  3886. windows overlapping consensus peaks for each histone mark, as well as the
  3887. \begin_inset Flex Glossary Term
  3888. status open
  3889. \begin_layout Plain Layout
  3890. RNA-seq
  3891. \end_layout
  3892. \end_inset
  3893. data, in order to identify patterns of coordinated variation across all
  3894. data sets
  3895. \begin_inset CommandInset citation
  3896. LatexCommand cite
  3897. key "Argelaguet2018"
  3898. literal "false"
  3899. \end_inset
  3900. .
  3901. The results are summarized in Figure
  3902. \begin_inset CommandInset ref
  3903. LatexCommand ref
  3904. reference "fig:MOFA-master"
  3905. plural "false"
  3906. caps "false"
  3907. noprefix "false"
  3908. \end_inset
  3909. .
  3910. \begin_inset Flex Glossary Term (Capital, pl)
  3911. status open
  3912. \begin_layout Plain Layout
  3913. LF
  3914. \end_layout
  3915. \end_inset
  3916. 1, 4, and 5 were determined to explain the most variation consistently
  3917. across all data sets (Figure
  3918. \begin_inset CommandInset ref
  3919. LatexCommand ref
  3920. reference "fig:mofa-varexplained"
  3921. plural "false"
  3922. caps "false"
  3923. noprefix "false"
  3924. \end_inset
  3925. ), and scatter plots of these factors show that they also correlate best
  3926. with the experimental factors (Figure
  3927. \begin_inset CommandInset ref
  3928. LatexCommand ref
  3929. reference "fig:mofa-lf-scatter"
  3930. plural "false"
  3931. caps "false"
  3932. noprefix "false"
  3933. \end_inset
  3934. ).
  3935. \begin_inset Flex Glossary Term
  3936. status open
  3937. \begin_layout Plain Layout
  3938. LF
  3939. \end_layout
  3940. \end_inset
  3941. 2 captures the batch effect in the
  3942. \begin_inset Flex Glossary Term
  3943. status open
  3944. \begin_layout Plain Layout
  3945. RNA-seq
  3946. \end_layout
  3947. \end_inset
  3948. data.
  3949. Removing the effect of
  3950. \begin_inset Flex Glossary Term
  3951. status open
  3952. \begin_layout Plain Layout
  3953. LF
  3954. \end_layout
  3955. \end_inset
  3956. 2 using
  3957. \begin_inset Flex Glossary Term
  3958. status open
  3959. \begin_layout Plain Layout
  3960. MOFA
  3961. \end_layout
  3962. \end_inset
  3963. theoretically yields a batch correction that does not depend on knowing
  3964. the experimental factors.
  3965. When this was attempted, the resulting batch correction was comparable
  3966. to ComBat (see Figure
  3967. \begin_inset CommandInset ref
  3968. LatexCommand ref
  3969. reference "fig:RNA-PCA-ComBat-batchsub"
  3970. plural "false"
  3971. caps "false"
  3972. noprefix "false"
  3973. \end_inset
  3974. ), indicating that the ComBat-based batch correction has little room for
  3975. improvement given the problems with the data set.
  3976. \end_layout
  3977. \begin_layout Standard
  3978. \begin_inset ERT
  3979. status open
  3980. \begin_layout Plain Layout
  3981. \backslash
  3982. afterpage{
  3983. \end_layout
  3984. \begin_layout Plain Layout
  3985. \backslash
  3986. begin{landscape}
  3987. \end_layout
  3988. \end_inset
  3989. \end_layout
  3990. \begin_layout Standard
  3991. \begin_inset Float figure
  3992. wide false
  3993. sideways false
  3994. status open
  3995. \begin_layout Plain Layout
  3996. \begin_inset Float figure
  3997. wide false
  3998. sideways false
  3999. status collapsed
  4000. \begin_layout Plain Layout
  4001. \align center
  4002. \begin_inset Graphics
  4003. filename graphics/CD4-csaw/MOFA-varExplaiend-matrix-CROP.png
  4004. lyxscale 25
  4005. width 45col%
  4006. groupId mofa-subfig
  4007. \end_inset
  4008. \end_layout
  4009. \begin_layout Plain Layout
  4010. \begin_inset Caption Standard
  4011. \begin_layout Plain Layout
  4012. \series bold
  4013. \begin_inset CommandInset label
  4014. LatexCommand label
  4015. name "fig:mofa-varexplained"
  4016. \end_inset
  4017. Variance explained in each data set by each latent factor estimated by MOFA.
  4018. \series default
  4019. For each LF learned by MOFA, the variance explained by that factor in each
  4020. data set (
  4021. \begin_inset Quotes eld
  4022. \end_inset
  4023. view
  4024. \begin_inset Quotes erd
  4025. \end_inset
  4026. ) is shown by the shading of the cells in the lower section.
  4027. The upper section shows the total fraction of each data set's variance
  4028. that is explained by all LFs combined.
  4029. \end_layout
  4030. \end_inset
  4031. \end_layout
  4032. \end_inset
  4033. \begin_inset space \hfill{}
  4034. \end_inset
  4035. \begin_inset Float figure
  4036. wide false
  4037. sideways false
  4038. status collapsed
  4039. \begin_layout Plain Layout
  4040. \align center
  4041. \begin_inset Graphics
  4042. filename graphics/CD4-csaw/MOFA-LF-scatter-small.png
  4043. lyxscale 25
  4044. width 45col%
  4045. groupId mofa-subfig
  4046. \end_inset
  4047. \end_layout
  4048. \begin_layout Plain Layout
  4049. \begin_inset Caption Standard
  4050. \begin_layout Plain Layout
  4051. \series bold
  4052. \begin_inset CommandInset label
  4053. LatexCommand label
  4054. name "fig:mofa-lf-scatter"
  4055. \end_inset
  4056. Scatter plots of specific pairs of MOFA latent factors.
  4057. \series default
  4058. LFs 1, 4, and 5 explain substantial variation in all data sets, so they
  4059. were plotted against each other in order to reveal patterns of variation
  4060. that are shared across all data sets.
  4061. These plots can be interpreted similarly to PCA and PCoA plots.
  4062. \end_layout
  4063. \end_inset
  4064. \end_layout
  4065. \end_inset
  4066. \end_layout
  4067. \begin_layout Plain Layout
  4068. \begin_inset Flex TODO Note (inline)
  4069. status open
  4070. \begin_layout Plain Layout
  4071. Figure font a bit too small
  4072. \end_layout
  4073. \end_inset
  4074. \end_layout
  4075. \begin_layout Plain Layout
  4076. \begin_inset Caption Standard
  4077. \begin_layout Plain Layout
  4078. \begin_inset Argument 1
  4079. status collapsed
  4080. \begin_layout Plain Layout
  4081. MOFA latent factors identify shared patterns of variation.
  4082. \end_layout
  4083. \end_inset
  4084. \begin_inset CommandInset label
  4085. LatexCommand label
  4086. name "fig:MOFA-master"
  4087. \end_inset
  4088. \series bold
  4089. MOFA latent factors identify shared patterns of variation.
  4090. \series default
  4091. MOFA was used to estimate latent factors (LFs) that explain substantial
  4092. variation in the RNA-seq data and the ChIP-seq data (a).
  4093. Then specific LFs of interest were selected and plotted (b).
  4094. \end_layout
  4095. \end_inset
  4096. \end_layout
  4097. \end_inset
  4098. \end_layout
  4099. \begin_layout Standard
  4100. \begin_inset ERT
  4101. status open
  4102. \begin_layout Plain Layout
  4103. \backslash
  4104. end{landscape}
  4105. \end_layout
  4106. \begin_layout Plain Layout
  4107. }
  4108. \end_layout
  4109. \end_inset
  4110. \end_layout
  4111. \begin_layout Standard
  4112. \begin_inset Note Note
  4113. status collapsed
  4114. \begin_layout Plain Layout
  4115. \begin_inset Float figure
  4116. wide false
  4117. sideways false
  4118. status open
  4119. \begin_layout Plain Layout
  4120. \align center
  4121. \begin_inset Graphics
  4122. filename graphics/CD4-csaw/MOFA-batch-correct-CROP.png
  4123. lyxscale 25
  4124. width 100col%
  4125. groupId colwidth-raster
  4126. \end_inset
  4127. \end_layout
  4128. \begin_layout Plain Layout
  4129. \begin_inset Caption Standard
  4130. \begin_layout Plain Layout
  4131. \series bold
  4132. \begin_inset CommandInset label
  4133. LatexCommand label
  4134. name "fig:mofa-batchsub"
  4135. \end_inset
  4136. Result of RNA-seq batch-correction using MOFA latent factors
  4137. \end_layout
  4138. \end_inset
  4139. \end_layout
  4140. \end_inset
  4141. \end_layout
  4142. \end_inset
  4143. \end_layout
  4144. \begin_layout Section
  4145. Results
  4146. \end_layout
  4147. \begin_layout Standard
  4148. \begin_inset Flex TODO Note (inline)
  4149. status open
  4150. \begin_layout Plain Layout
  4151. Focus on what hypotheses were tested, then select figures that show how
  4152. those hypotheses were tested, even if the result is a negative.
  4153. Not every interesting result needs to be in here.
  4154. Chapter should tell a story.
  4155. \end_layout
  4156. \end_inset
  4157. \end_layout
  4158. \begin_layout Subsection
  4159. Interpretation of RNA-seq analysis is limited by a major confounding factor
  4160. \end_layout
  4161. \begin_layout Standard
  4162. Genes called as present in the
  4163. \begin_inset Flex Glossary Term
  4164. status open
  4165. \begin_layout Plain Layout
  4166. RNA-seq
  4167. \end_layout
  4168. \end_inset
  4169. data were tested for differential expression between all time points and
  4170. cell types.
  4171. The counts of differentially expressed genes are shown in Table
  4172. \begin_inset CommandInset ref
  4173. LatexCommand ref
  4174. reference "tab:Estimated-and-detected-rnaseq"
  4175. plural "false"
  4176. caps "false"
  4177. noprefix "false"
  4178. \end_inset
  4179. .
  4180. Notably, all the results for Day 0 and Day 5 have substantially fewer genes
  4181. called differentially expressed than any of the results for other time
  4182. points.
  4183. This is an unfortunate result of the difference in sample quality between
  4184. the two batches of
  4185. \begin_inset Flex Glossary Term
  4186. status open
  4187. \begin_layout Plain Layout
  4188. RNA-seq
  4189. \end_layout
  4190. \end_inset
  4191. data.
  4192. All the samples in Batch 1, which includes all the samples from Days 0
  4193. and 5, have substantially more variability than the samples in Batch 2,
  4194. which includes the other time points.
  4195. This is reflected in the substantially higher weights assigned to Batch
  4196. 2 (Figure
  4197. \begin_inset CommandInset ref
  4198. LatexCommand ref
  4199. reference "fig:RNA-seq-weights-vs-covars"
  4200. plural "false"
  4201. caps "false"
  4202. noprefix "false"
  4203. \end_inset
  4204. ).
  4205. \begin_inset Float table
  4206. wide false
  4207. sideways false
  4208. status collapsed
  4209. \begin_layout Plain Layout
  4210. \align center
  4211. \begin_inset Tabular
  4212. <lyxtabular version="3" rows="11" columns="3">
  4213. <features tabularvalignment="middle">
  4214. <column alignment="center" valignment="top">
  4215. <column alignment="center" valignment="top">
  4216. <column alignment="center" valignment="top">
  4217. <row>
  4218. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  4219. \begin_inset Text
  4220. \begin_layout Plain Layout
  4221. Test
  4222. \end_layout
  4223. \end_inset
  4224. </cell>
  4225. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  4226. \begin_inset Text
  4227. \begin_layout Plain Layout
  4228. Est.
  4229. non-null
  4230. \end_layout
  4231. \end_inset
  4232. </cell>
  4233. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" rightline="true" usebox="none">
  4234. \begin_inset Text
  4235. \begin_layout Plain Layout
  4236. \begin_inset Formula $\mathrm{FDR}\le10\%$
  4237. \end_inset
  4238. \end_layout
  4239. \end_inset
  4240. </cell>
  4241. </row>
  4242. <row>
  4243. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4244. \begin_inset Text
  4245. \begin_layout Plain Layout
  4246. Naïve Day 0 vs Day 1
  4247. \end_layout
  4248. \end_inset
  4249. </cell>
  4250. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4251. \begin_inset Text
  4252. \begin_layout Plain Layout
  4253. 5992
  4254. \end_layout
  4255. \end_inset
  4256. </cell>
  4257. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  4258. \begin_inset Text
  4259. \begin_layout Plain Layout
  4260. 1613
  4261. \end_layout
  4262. \end_inset
  4263. </cell>
  4264. </row>
  4265. <row>
  4266. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4267. \begin_inset Text
  4268. \begin_layout Plain Layout
  4269. Naïve Day 0 vs Day 5
  4270. \end_layout
  4271. \end_inset
  4272. </cell>
  4273. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4274. \begin_inset Text
  4275. \begin_layout Plain Layout
  4276. 3038
  4277. \end_layout
  4278. \end_inset
  4279. </cell>
  4280. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  4281. \begin_inset Text
  4282. \begin_layout Plain Layout
  4283. 32
  4284. \end_layout
  4285. \end_inset
  4286. </cell>
  4287. </row>
  4288. <row>
  4289. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4290. \begin_inset Text
  4291. \begin_layout Plain Layout
  4292. Naïve Day 0 vs Day 14
  4293. \end_layout
  4294. \end_inset
  4295. </cell>
  4296. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4297. \begin_inset Text
  4298. \begin_layout Plain Layout
  4299. 1870
  4300. \end_layout
  4301. \end_inset
  4302. </cell>
  4303. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  4304. \begin_inset Text
  4305. \begin_layout Plain Layout
  4306. 190
  4307. \end_layout
  4308. \end_inset
  4309. </cell>
  4310. </row>
  4311. <row>
  4312. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4313. \begin_inset Text
  4314. \begin_layout Plain Layout
  4315. Memory Day 0 vs Day 1
  4316. \end_layout
  4317. \end_inset
  4318. </cell>
  4319. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4320. \begin_inset Text
  4321. \begin_layout Plain Layout
  4322. 3195
  4323. \end_layout
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  4325. </cell>
  4326. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  4327. \begin_inset Text
  4328. \begin_layout Plain Layout
  4329. 411
  4330. \end_layout
  4331. \end_inset
  4332. </cell>
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  4334. <row>
  4335. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4336. \begin_inset Text
  4337. \begin_layout Plain Layout
  4338. Memory Day 0 vs Day 5
  4339. \end_layout
  4340. \end_inset
  4341. </cell>
  4342. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4343. \begin_inset Text
  4344. \begin_layout Plain Layout
  4345. 2688
  4346. \end_layout
  4347. \end_inset
  4348. </cell>
  4349. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  4350. \begin_inset Text
  4351. \begin_layout Plain Layout
  4352. 18
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  4358. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4359. \begin_inset Text
  4360. \begin_layout Plain Layout
  4361. Memory Day 0 vs Day 14
  4362. \end_layout
  4363. \end_inset
  4364. </cell>
  4365. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4366. \begin_inset Text
  4367. \begin_layout Plain Layout
  4368. 1911
  4369. \end_layout
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  4371. </cell>
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  4373. \begin_inset Text
  4374. \begin_layout Plain Layout
  4375. 227
  4376. \end_layout
  4377. \end_inset
  4378. </cell>
  4379. </row>
  4380. <row>
  4381. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4382. \begin_inset Text
  4383. \begin_layout Plain Layout
  4384. Day 0 Naïve vs Memory
  4385. \end_layout
  4386. \end_inset
  4387. </cell>
  4388. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4389. \begin_inset Text
  4390. \begin_layout Plain Layout
  4391. 0
  4392. \end_layout
  4393. \end_inset
  4394. </cell>
  4395. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  4396. \begin_inset Text
  4397. \begin_layout Plain Layout
  4398. 2
  4399. \end_layout
  4400. \end_inset
  4401. </cell>
  4402. </row>
  4403. <row>
  4404. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4405. \begin_inset Text
  4406. \begin_layout Plain Layout
  4407. Day 1 Naïve vs Memory
  4408. \end_layout
  4409. \end_inset
  4410. </cell>
  4411. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4412. \begin_inset Text
  4413. \begin_layout Plain Layout
  4414. 9167
  4415. \end_layout
  4416. \end_inset
  4417. </cell>
  4418. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  4419. \begin_inset Text
  4420. \begin_layout Plain Layout
  4421. 5532
  4422. \end_layout
  4423. \end_inset
  4424. </cell>
  4425. </row>
  4426. <row>
  4427. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4428. \begin_inset Text
  4429. \begin_layout Plain Layout
  4430. Day 5 Naïve vs Memory
  4431. \end_layout
  4432. \end_inset
  4433. </cell>
  4434. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4435. \begin_inset Text
  4436. \begin_layout Plain Layout
  4437. 0
  4438. \end_layout
  4439. \end_inset
  4440. </cell>
  4441. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  4442. \begin_inset Text
  4443. \begin_layout Plain Layout
  4444. 0
  4445. \end_layout
  4446. \end_inset
  4447. </cell>
  4448. </row>
  4449. <row>
  4450. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  4451. \begin_inset Text
  4452. \begin_layout Plain Layout
  4453. Day 14 Naïve vs Memory
  4454. \end_layout
  4455. \end_inset
  4456. </cell>
  4457. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  4458. \begin_inset Text
  4459. \begin_layout Plain Layout
  4460. 6446
  4461. \end_layout
  4462. \end_inset
  4463. </cell>
  4464. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" rightline="true" usebox="none">
  4465. \begin_inset Text
  4466. \begin_layout Plain Layout
  4467. 2319
  4468. \end_layout
  4469. \end_inset
  4470. </cell>
  4471. </row>
  4472. </lyxtabular>
  4473. \end_inset
  4474. \end_layout
  4475. \begin_layout Plain Layout
  4476. \begin_inset Caption Standard
  4477. \begin_layout Plain Layout
  4478. \begin_inset Argument 1
  4479. status collapsed
  4480. \begin_layout Plain Layout
  4481. Estimated and detected differentially expressed genes.
  4482. \end_layout
  4483. \end_inset
  4484. \begin_inset CommandInset label
  4485. LatexCommand label
  4486. name "tab:Estimated-and-detected-rnaseq"
  4487. \end_inset
  4488. \series bold
  4489. Estimated and detected differentially expressed genes.
  4490. \series default
  4491. \begin_inset Quotes eld
  4492. \end_inset
  4493. Test
  4494. \begin_inset Quotes erd
  4495. \end_inset
  4496. : Which sample groups were compared;
  4497. \begin_inset Quotes eld
  4498. \end_inset
  4499. Est non-null
  4500. \begin_inset Quotes erd
  4501. \end_inset
  4502. : Estimated number of differentially expressed genes, using the method of
  4503. averaging local FDR values
  4504. \begin_inset CommandInset citation
  4505. LatexCommand cite
  4506. key "Phipson2013Thesis"
  4507. literal "false"
  4508. \end_inset
  4509. ;
  4510. \begin_inset Quotes eld
  4511. \end_inset
  4512. \begin_inset Formula $\mathrm{FDR}\le10\%$
  4513. \end_inset
  4514. \begin_inset Quotes erd
  4515. \end_inset
  4516. : Number of significantly differentially expressed genes at an FDR threshold
  4517. of 10%.
  4518. The total number of genes tested was 16707.
  4519. \end_layout
  4520. \end_inset
  4521. \end_layout
  4522. \end_inset
  4523. \begin_inset Note Note
  4524. status collapsed
  4525. \begin_layout Plain Layout
  4526. If float lost issues, reposition randomly until success.
  4527. \end_layout
  4528. \end_inset
  4529. The batch effect has both a systematic component and a random noise component.
  4530. While the systematic component was subtracted out using ComBat (Figure
  4531. \begin_inset CommandInset ref
  4532. LatexCommand ref
  4533. reference "fig:RNA-PCA"
  4534. plural "false"
  4535. caps "false"
  4536. noprefix "false"
  4537. \end_inset
  4538. ), no such correction is possible for the noise component: Batch 1 simply
  4539. has substantially more random noise in it, which reduces the statistical
  4540. power for any differential expression tests involving samples in that batch.
  4541. \end_layout
  4542. \begin_layout Standard
  4543. Despite the difficulty in detecting specific differentially expressed genes,
  4544. there is still evidence that differential expression is present for these
  4545. time points.
  4546. In Figure
  4547. \begin_inset CommandInset ref
  4548. LatexCommand ref
  4549. reference "fig:rna-pca-final"
  4550. plural "false"
  4551. caps "false"
  4552. noprefix "false"
  4553. \end_inset
  4554. , there is a clear separation between naïve and memory samples at Day 0,
  4555. despite the fact that only 2 genes were significantly differentially expressed
  4556. for this comparison.
  4557. Similarly, the small numbers of genes detected for the Day 0 vs Day 5 compariso
  4558. ns do not reflect the large separation between these time points in Figure
  4559. \begin_inset CommandInset ref
  4560. LatexCommand ref
  4561. reference "fig:rna-pca-final"
  4562. plural "false"
  4563. caps "false"
  4564. noprefix "false"
  4565. \end_inset
  4566. .
  4567. In addition, the
  4568. \begin_inset Flex Glossary Term
  4569. status open
  4570. \begin_layout Plain Layout
  4571. MOFA
  4572. \end_layout
  4573. \end_inset
  4574. \begin_inset Flex Glossary Term
  4575. status open
  4576. \begin_layout Plain Layout
  4577. LF
  4578. \end_layout
  4579. \end_inset
  4580. plots in Figure
  4581. \begin_inset CommandInset ref
  4582. LatexCommand ref
  4583. reference "fig:mofa-lf-scatter"
  4584. plural "false"
  4585. caps "false"
  4586. noprefix "false"
  4587. \end_inset
  4588. .
  4589. This suggests that there is indeed a differential expression signal present
  4590. in the data for these comparisons, but the large variability in the Batch
  4591. 1 samples obfuscates this signal at the individual gene level.
  4592. As a result, it is impossible to make any meaningful statements about the
  4593. \begin_inset Quotes eld
  4594. \end_inset
  4595. size
  4596. \begin_inset Quotes erd
  4597. \end_inset
  4598. of the gene signature for any time point, since the number of significant
  4599. genes as well as the estimated number of differentially expressed genes
  4600. depends so strongly on the variations in sample quality in addition to
  4601. the size of the differential expression signal in the data.
  4602. Gene-set enrichment analyses are similarly impractical.
  4603. However, analyses looking at genome-wide patterns of expression are still
  4604. practical.
  4605. \end_layout
  4606. \begin_layout Standard
  4607. \begin_inset Float figure
  4608. wide false
  4609. sideways false
  4610. status collapsed
  4611. \begin_layout Plain Layout
  4612. \align center
  4613. \begin_inset Graphics
  4614. filename graphics/CD4-csaw/RNA-seq/PCA-final-12-CROP.png
  4615. lyxscale 25
  4616. width 100col%
  4617. groupId colwidth-raster
  4618. \end_inset
  4619. \end_layout
  4620. \begin_layout Plain Layout
  4621. \begin_inset Caption Standard
  4622. \begin_layout Plain Layout
  4623. \begin_inset Argument 1
  4624. status collapsed
  4625. \begin_layout Plain Layout
  4626. PCoA plot of RNA-seq samples after ComBat batch correction.
  4627. \end_layout
  4628. \end_inset
  4629. \begin_inset CommandInset label
  4630. LatexCommand label
  4631. name "fig:rna-pca-final"
  4632. \end_inset
  4633. \series bold
  4634. PCoA plot of RNA-seq samples after ComBat batch correction.
  4635. \series default
  4636. Each point represents an individual sample.
  4637. Samples with the same combination of cell type and time point are encircled
  4638. with a shaded region to aid in visual identification of the sample groups.
  4639. Samples of the same cell type from the same donor are connected by lines
  4640. to indicate the
  4641. \begin_inset Quotes eld
  4642. \end_inset
  4643. trajectory
  4644. \begin_inset Quotes erd
  4645. \end_inset
  4646. of each donor's cells over time in PCoA space.
  4647. \end_layout
  4648. \end_inset
  4649. \end_layout
  4650. \end_inset
  4651. \end_layout
  4652. \begin_layout Subsection
  4653. H3K4 and H3K27 methylation occur in broad regions and are enriched near
  4654. promoters
  4655. \end_layout
  4656. \begin_layout Standard
  4657. \begin_inset Float table
  4658. wide false
  4659. sideways false
  4660. status open
  4661. \begin_layout Plain Layout
  4662. \align center
  4663. \begin_inset Flex TODO Note (inline)
  4664. status open
  4665. \begin_layout Plain Layout
  4666. Also get
  4667. \emph on
  4668. median
  4669. \emph default
  4670. peak width and maybe other quantiles (25%, 75%)
  4671. \end_layout
  4672. \end_inset
  4673. \end_layout
  4674. \begin_layout Plain Layout
  4675. \align center
  4676. \begin_inset Tabular
  4677. <lyxtabular version="3" rows="4" columns="5">
  4678. <features tabularvalignment="middle">
  4679. <column alignment="center" valignment="top">
  4680. <column alignment="center" valignment="top">
  4681. <column alignment="center" valignment="top">
  4682. <column alignment="center" valignment="top">
  4683. <column alignment="center" valignment="top">
  4684. <row>
  4685. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  4686. \begin_inset Text
  4687. \begin_layout Plain Layout
  4688. Histone Mark
  4689. \end_layout
  4690. \end_inset
  4691. </cell>
  4692. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  4693. \begin_inset Text
  4694. \begin_layout Plain Layout
  4695. # Peaks
  4696. \end_layout
  4697. \end_inset
  4698. </cell>
  4699. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  4700. \begin_inset Text
  4701. \begin_layout Plain Layout
  4702. Mean peak width
  4703. \end_layout
  4704. \end_inset
  4705. </cell>
  4706. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  4707. \begin_inset Text
  4708. \begin_layout Plain Layout
  4709. genome coverage
  4710. \end_layout
  4711. \end_inset
  4712. </cell>
  4713. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" rightline="true" usebox="none">
  4714. \begin_inset Text
  4715. \begin_layout Plain Layout
  4716. FRiP
  4717. \end_layout
  4718. \end_inset
  4719. </cell>
  4720. </row>
  4721. <row>
  4722. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4723. \begin_inset Text
  4724. \begin_layout Plain Layout
  4725. H3K4me2
  4726. \end_layout
  4727. \end_inset
  4728. </cell>
  4729. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4730. \begin_inset Text
  4731. \begin_layout Plain Layout
  4732. 14,965
  4733. \end_layout
  4734. \end_inset
  4735. </cell>
  4736. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4737. \begin_inset Text
  4738. \begin_layout Plain Layout
  4739. 3,970
  4740. \end_layout
  4741. \end_inset
  4742. </cell>
  4743. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4744. \begin_inset Text
  4745. \begin_layout Plain Layout
  4746. 1.92%
  4747. \end_layout
  4748. \end_inset
  4749. </cell>
  4750. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  4751. \begin_inset Text
  4752. \begin_layout Plain Layout
  4753. 14.2%
  4754. \end_layout
  4755. \end_inset
  4756. </cell>
  4757. </row>
  4758. <row>
  4759. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4760. \begin_inset Text
  4761. \begin_layout Plain Layout
  4762. H3K4me3
  4763. \end_layout
  4764. \end_inset
  4765. </cell>
  4766. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4767. \begin_inset Text
  4768. \begin_layout Plain Layout
  4769. 6,163
  4770. \end_layout
  4771. \end_inset
  4772. </cell>
  4773. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4774. \begin_inset Text
  4775. \begin_layout Plain Layout
  4776. 2,946
  4777. \end_layout
  4778. \end_inset
  4779. </cell>
  4780. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  4781. \begin_inset Text
  4782. \begin_layout Plain Layout
  4783. 0.588%
  4784. \end_layout
  4785. \end_inset
  4786. </cell>
  4787. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  4788. \begin_inset Text
  4789. \begin_layout Plain Layout
  4790. 6.57%
  4791. \end_layout
  4792. \end_inset
  4793. </cell>
  4794. </row>
  4795. <row>
  4796. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  4797. \begin_inset Text
  4798. \begin_layout Plain Layout
  4799. H3K27me3
  4800. \end_layout
  4801. \end_inset
  4802. </cell>
  4803. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  4804. \begin_inset Text
  4805. \begin_layout Plain Layout
  4806. 18,139
  4807. \end_layout
  4808. \end_inset
  4809. </cell>
  4810. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  4811. \begin_inset Text
  4812. \begin_layout Plain Layout
  4813. 18,967
  4814. \end_layout
  4815. \end_inset
  4816. </cell>
  4817. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  4818. \begin_inset Text
  4819. \begin_layout Plain Layout
  4820. 11.1%
  4821. \end_layout
  4822. \end_inset
  4823. </cell>
  4824. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" rightline="true" usebox="none">
  4825. \begin_inset Text
  4826. \begin_layout Plain Layout
  4827. 22.5%
  4828. \end_layout
  4829. \end_inset
  4830. </cell>
  4831. </row>
  4832. </lyxtabular>
  4833. \end_inset
  4834. \end_layout
  4835. \begin_layout Plain Layout
  4836. \begin_inset Flex TODO Note (inline)
  4837. status open
  4838. \begin_layout Plain Layout
  4839. Get the IDR threshold
  4840. \end_layout
  4841. \end_inset
  4842. \end_layout
  4843. \begin_layout Plain Layout
  4844. \begin_inset Caption Standard
  4845. \begin_layout Plain Layout
  4846. \begin_inset Argument 1
  4847. status collapsed
  4848. \begin_layout Plain Layout
  4849. Summary of peak-calling statistics.
  4850. \end_layout
  4851. \end_inset
  4852. \begin_inset CommandInset label
  4853. LatexCommand label
  4854. name "tab:peak-calling-summary"
  4855. \end_inset
  4856. \series bold
  4857. Summary of peak-calling statistics.
  4858. \series default
  4859. For each histone mark, the number of peaks called using SICER at an IDR
  4860. threshold of ???, the mean width of those peaks, the fraction of the genome
  4861. covered by peaks, and the fraction of reads in peaks (FRiP).
  4862. \end_layout
  4863. \end_inset
  4864. \end_layout
  4865. \end_inset
  4866. \end_layout
  4867. \begin_layout Standard
  4868. Table
  4869. \begin_inset CommandInset ref
  4870. LatexCommand ref
  4871. reference "tab:peak-calling-summary"
  4872. plural "false"
  4873. caps "false"
  4874. noprefix "false"
  4875. \end_inset
  4876. gives a summary of the peak calling statistics for each histone mark.
  4877. Consistent with previous observations, all 3 histone marks occur in broad
  4878. regions spanning many consecutive nucleosomes, rather than in sharp peaks
  4879. as would be expected for a transcription factor or other molecule that
  4880. binds to specific sites.
  4881. This conclusion is further supported by Figure
  4882. \begin_inset CommandInset ref
  4883. LatexCommand ref
  4884. reference "fig:CCF-with-blacklist"
  4885. plural "false"
  4886. caps "false"
  4887. noprefix "false"
  4888. \end_inset
  4889. , in which a clear nucleosome-sized periodicity is visible in the cross-correlat
  4890. ion value for each sample, indicating that each time a given mark is present
  4891. on one histone, it is also likely to be found on adjacent histones as well.
  4892. H3K27me3 enrichment in particular is substantially more broad than either
  4893. H3K4 mark, with a mean peak width of almost 19,000 bp.
  4894. This is also reflected in the periodicity observed in Figure
  4895. \begin_inset CommandInset ref
  4896. LatexCommand ref
  4897. reference "fig:CCF-with-blacklist"
  4898. plural "false"
  4899. caps "false"
  4900. noprefix "false"
  4901. \end_inset
  4902. , which remains strong much farther out for H3K27me3 than the other marks,
  4903. showing H3K27me3 especially tends to be found on long runs of consecutive
  4904. histones.
  4905. \end_layout
  4906. \begin_layout Standard
  4907. \begin_inset Flex TODO Note (inline)
  4908. status open
  4909. \begin_layout Plain Layout
  4910. \end_layout
  4911. \end_inset
  4912. \end_layout
  4913. \begin_layout Standard
  4914. All 3 histone marks tend to occur more often near promoter regions, as shown
  4915. in Figure
  4916. \begin_inset CommandInset ref
  4917. LatexCommand ref
  4918. reference "fig:near-promoter-peak-enrich"
  4919. plural "false"
  4920. caps "false"
  4921. noprefix "false"
  4922. \end_inset
  4923. .
  4924. The majority of each density distribution is flat, representing the background
  4925. density of peaks genome-wide.
  4926. Each distribution has a peak near zero, representing an enrichment of peaks
  4927. close to
  4928. \begin_inset Flex Glossary Term
  4929. status open
  4930. \begin_layout Plain Layout
  4931. TSS
  4932. \end_layout
  4933. \end_inset
  4934. positions relative to the remainder of the genome.
  4935. Interestingly, the
  4936. \begin_inset Quotes eld
  4937. \end_inset
  4938. radius
  4939. \begin_inset Quotes erd
  4940. \end_inset
  4941. within which this enrichment occurs is not the same for every histone mark
  4942. (Table
  4943. \begin_inset CommandInset ref
  4944. LatexCommand ref
  4945. reference "tab:effective-promoter-radius"
  4946. plural "false"
  4947. caps "false"
  4948. noprefix "false"
  4949. \end_inset
  4950. ).
  4951. For H3K4me2 and H3K4me3, peaks are most enriched within 1
  4952. \begin_inset space ~
  4953. \end_inset
  4954. kbp of
  4955. \begin_inset Flex Glossary Term
  4956. status open
  4957. \begin_layout Plain Layout
  4958. TSS
  4959. \end_layout
  4960. \end_inset
  4961. positions, while for H3K27me3, enrichment is broader, extending to 2.5
  4962. \begin_inset space ~
  4963. \end_inset
  4964. kbp.
  4965. These
  4966. \begin_inset Quotes eld
  4967. \end_inset
  4968. effective promoter radii
  4969. \begin_inset Quotes erd
  4970. \end_inset
  4971. remain approximately the same across all combinations of experimental condition
  4972. (cell type, time point, and donor), so they appear to be a property of
  4973. the histone mark itself.
  4974. Hence, these radii were used to define the promoter regions for each histone
  4975. mark in all further analyses.
  4976. \end_layout
  4977. \begin_layout Standard
  4978. \begin_inset Float figure
  4979. wide false
  4980. sideways false
  4981. status open
  4982. \begin_layout Plain Layout
  4983. \align center
  4984. \begin_inset Graphics
  4985. filename graphics/CD4-csaw/Promoter-Peak-Distance-Profile-PAGE1-CROP.pdf
  4986. lyxscale 50
  4987. width 80col%
  4988. \end_inset
  4989. \end_layout
  4990. \begin_layout Plain Layout
  4991. \begin_inset Flex TODO Note (inline)
  4992. status open
  4993. \begin_layout Plain Layout
  4994. Future direction idea: Need a control: shuffle all peaks and repeat, N times.
  4995. \end_layout
  4996. \end_inset
  4997. \end_layout
  4998. \begin_layout Plain Layout
  4999. \begin_inset Caption Standard
  5000. \begin_layout Plain Layout
  5001. \begin_inset Argument 1
  5002. status collapsed
  5003. \begin_layout Plain Layout
  5004. Enrichment of peaks in promoter neighborhoods.
  5005. \end_layout
  5006. \end_inset
  5007. \begin_inset CommandInset label
  5008. LatexCommand label
  5009. name "fig:near-promoter-peak-enrich"
  5010. \end_inset
  5011. \series bold
  5012. Enrichment of peaks in promoter neighborhoods.
  5013. \series default
  5014. This plot shows the distribution of distances from each annotated transcription
  5015. start site in the genome to the nearest called peak.
  5016. Each line represents one combination of histone mark, cell type, and time
  5017. point.
  5018. Distributions are smoothed using kernel density estimation.
  5019. TSSs that occur
  5020. \emph on
  5021. within
  5022. \emph default
  5023. peaks were excluded from this plot to avoid a large spike at zero that
  5024. would overshadow the rest of the distribution.
  5025. (Note: this figure was generated using the original peak calls and expression
  5026. values from
  5027. \begin_inset Flex Glossary Term
  5028. status open
  5029. \begin_layout Plain Layout
  5030. GEO
  5031. \end_layout
  5032. \end_inset
  5033. \begin_inset CommandInset citation
  5034. LatexCommand cite
  5035. key "LaMere2016"
  5036. literal "false"
  5037. \end_inset
  5038. .)
  5039. \end_layout
  5040. \end_inset
  5041. \end_layout
  5042. \end_inset
  5043. \end_layout
  5044. \begin_layout Standard
  5045. \begin_inset Float table
  5046. wide false
  5047. sideways false
  5048. status collapsed
  5049. \begin_layout Plain Layout
  5050. \align center
  5051. \begin_inset Tabular
  5052. <lyxtabular version="3" rows="4" columns="2">
  5053. <features tabularvalignment="middle">
  5054. <column alignment="center" valignment="top">
  5055. <column alignment="center" valignment="top">
  5056. <row>
  5057. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  5058. \begin_inset Text
  5059. \begin_layout Plain Layout
  5060. Histone mark
  5061. \end_layout
  5062. \end_inset
  5063. </cell>
  5064. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" rightline="true" usebox="none">
  5065. \begin_inset Text
  5066. \begin_layout Plain Layout
  5067. Effective promoter radius
  5068. \end_layout
  5069. \end_inset
  5070. </cell>
  5071. </row>
  5072. <row>
  5073. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  5074. \begin_inset Text
  5075. \begin_layout Plain Layout
  5076. H3K4me2
  5077. \end_layout
  5078. \end_inset
  5079. </cell>
  5080. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
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  5083. 1 kb
  5084. \end_layout
  5085. \end_inset
  5086. </cell>
  5087. </row>
  5088. <row>
  5089. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  5090. \begin_inset Text
  5091. \begin_layout Plain Layout
  5092. H3K4me3
  5093. \end_layout
  5094. \end_inset
  5095. </cell>
  5096. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  5097. \begin_inset Text
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  5099. 1 kb
  5100. \end_layout
  5101. \end_inset
  5102. </cell>
  5103. </row>
  5104. <row>
  5105. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  5106. \begin_inset Text
  5107. \begin_layout Plain Layout
  5108. H3K27me3
  5109. \end_layout
  5110. \end_inset
  5111. </cell>
  5112. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" rightline="true" usebox="none">
  5113. \begin_inset Text
  5114. \begin_layout Plain Layout
  5115. 2.5 kb
  5116. \end_layout
  5117. \end_inset
  5118. </cell>
  5119. </row>
  5120. </lyxtabular>
  5121. \end_inset
  5122. \end_layout
  5123. \begin_layout Plain Layout
  5124. \begin_inset Caption Standard
  5125. \begin_layout Plain Layout
  5126. \begin_inset Argument 1
  5127. status collapsed
  5128. \begin_layout Plain Layout
  5129. Effective promoter radius for each histone mark.
  5130. \end_layout
  5131. \end_inset
  5132. \begin_inset CommandInset label
  5133. LatexCommand label
  5134. name "tab:effective-promoter-radius"
  5135. \end_inset
  5136. \series bold
  5137. Effective promoter radius for each histone mark.
  5138. \series default
  5139. These values represent the approximate distance from transcription start
  5140. site positions within which an excess of peaks are found, as shown in Figure
  5141. \begin_inset CommandInset ref
  5142. LatexCommand ref
  5143. reference "fig:near-promoter-peak-enrich"
  5144. plural "false"
  5145. caps "false"
  5146. noprefix "false"
  5147. \end_inset
  5148. .
  5149. \end_layout
  5150. \end_inset
  5151. \end_layout
  5152. \end_inset
  5153. \end_layout
  5154. \begin_layout Standard
  5155. \begin_inset Flex TODO Note (inline)
  5156. status open
  5157. \begin_layout Plain Layout
  5158. Consider also showing figure for distance to nearest peak center, and reference
  5159. median peak size once that is known.
  5160. \end_layout
  5161. \end_inset
  5162. \end_layout
  5163. \begin_layout Subsection
  5164. H3K4 and H3K27 promoter methylation has broadly the expected correlation
  5165. with gene expression
  5166. \end_layout
  5167. \begin_layout Standard
  5168. H3K4me2 and H3K4me2 have previously been reported as activating marks whose
  5169. presence in a gene's promoter is associated with higher gene expression,
  5170. while H3K27me3 has been reported as inactivating
  5171. \begin_inset CommandInset citation
  5172. LatexCommand cite
  5173. key "LaMere2016,LaMere2017"
  5174. literal "false"
  5175. \end_inset
  5176. .
  5177. The data are consistent with this characterization: genes whose promoters
  5178. (as defined by the radii for each histone mark listed in
  5179. \begin_inset CommandInset ref
  5180. LatexCommand ref
  5181. reference "tab:effective-promoter-radius"
  5182. plural "false"
  5183. caps "false"
  5184. noprefix "false"
  5185. \end_inset
  5186. ) overlap with a H3K4me2 or H3K4me3 peak tend to have higher expression
  5187. than those that don't, while H3K27me3 is likewise associated with lower
  5188. gene expression, as shown in
  5189. \begin_inset CommandInset ref
  5190. LatexCommand ref
  5191. reference "fig:fpkm-by-peak"
  5192. plural "false"
  5193. caps "false"
  5194. noprefix "false"
  5195. \end_inset
  5196. .
  5197. This pattern holds across all combinations of cell type and time point
  5198. (Welch's
  5199. \emph on
  5200. t
  5201. \emph default
  5202. -test, all
  5203. \begin_inset Formula $p\mathrm{-values}\ll2.2\times10^{-16}$
  5204. \end_inset
  5205. ).
  5206. The difference in average
  5207. \begin_inset Formula $\log_{2}$
  5208. \end_inset
  5209. \begin_inset Flex Glossary Term
  5210. status open
  5211. \begin_layout Plain Layout
  5212. FPKM
  5213. \end_layout
  5214. \end_inset
  5215. values when a peak overlaps the promoter is about
  5216. \begin_inset Formula $+5.67$
  5217. \end_inset
  5218. for H3K4me2,
  5219. \begin_inset Formula $+5.76$
  5220. \end_inset
  5221. for H3K4me2, and
  5222. \begin_inset Formula $-4.00$
  5223. \end_inset
  5224. for H3K27me3.
  5225. \end_layout
  5226. \begin_layout Standard
  5227. \begin_inset ERT
  5228. status open
  5229. \begin_layout Plain Layout
  5230. \backslash
  5231. afterpage{
  5232. \end_layout
  5233. \begin_layout Plain Layout
  5234. \backslash
  5235. begin{landscape}
  5236. \end_layout
  5237. \end_inset
  5238. \end_layout
  5239. \begin_layout Standard
  5240. \begin_inset Float figure
  5241. wide false
  5242. sideways false
  5243. status collapsed
  5244. \begin_layout Plain Layout
  5245. \align center
  5246. \begin_inset Graphics
  5247. filename graphics/CD4-csaw/FPKM-by-Peak-Violin-Plots-CROP.pdf
  5248. lyxscale 50
  5249. height 80theight%
  5250. \end_inset
  5251. \end_layout
  5252. \begin_layout Plain Layout
  5253. \begin_inset Caption Standard
  5254. \begin_layout Plain Layout
  5255. \begin_inset Argument 1
  5256. status collapsed
  5257. \begin_layout Plain Layout
  5258. Expression distributions of genes with and without promoter peaks.
  5259. \end_layout
  5260. \end_inset
  5261. \begin_inset CommandInset label
  5262. LatexCommand label
  5263. name "fig:fpkm-by-peak"
  5264. \end_inset
  5265. \series bold
  5266. Expression distributions of genes with and without promoter peaks.
  5267. \series default
  5268. For each histone mark in each experimental condition, the average RNA-seq
  5269. abundance (
  5270. \begin_inset Formula $\log_{2}$
  5271. \end_inset
  5272. FPKM) of each gene across all 4 donors was calculated.
  5273. Genes were grouped based on whether or not a peak was called in their promoters
  5274. in that condition, and the distribution of abundance values was plotted
  5275. for the no-peak and peak groups.
  5276. (Note: this figure was generated using the original peak calls and expression
  5277. values from
  5278. \begin_inset Flex Glossary Term
  5279. status open
  5280. \begin_layout Plain Layout
  5281. GEO
  5282. \end_layout
  5283. \end_inset
  5284. \begin_inset CommandInset citation
  5285. LatexCommand cite
  5286. key "LaMere2016"
  5287. literal "false"
  5288. \end_inset
  5289. .)
  5290. \end_layout
  5291. \end_inset
  5292. \end_layout
  5293. \end_inset
  5294. \end_layout
  5295. \begin_layout Standard
  5296. \begin_inset ERT
  5297. status open
  5298. \begin_layout Plain Layout
  5299. \backslash
  5300. end{landscape}
  5301. \end_layout
  5302. \begin_layout Plain Layout
  5303. }
  5304. \end_layout
  5305. \end_inset
  5306. \end_layout
  5307. \begin_layout Subsection
  5308. Gene expression and promoter histone methylation patterns show convergence
  5309. between naïve and memory cells at day 14
  5310. \end_layout
  5311. \begin_layout Standard
  5312. We hypothesized that if naïve cells had differentiated into memory cells
  5313. by Day 14, then their patterns of expression and histone modification should
  5314. converge with those of memory cells at Day 14.
  5315. Figure
  5316. \begin_inset CommandInset ref
  5317. LatexCommand ref
  5318. reference "fig:PCoA-promoters"
  5319. plural "false"
  5320. caps "false"
  5321. noprefix "false"
  5322. \end_inset
  5323. shows the patterns of variation in all 3 histone marks in the promoter
  5324. regions of the genome using
  5325. \begin_inset Flex Glossary Term
  5326. status open
  5327. \begin_layout Plain Layout
  5328. PCoA
  5329. \end_layout
  5330. \end_inset
  5331. .
  5332. All 3 marks show a noticeable convergence between the naïve and memory
  5333. samples at day 14, visible as an overlapping of the day 14 groups on each
  5334. plot.
  5335. This is consistent with the counts of significantly differentially modified
  5336. promoters and estimates of the total numbers of differentially modified
  5337. promoters shown in Table
  5338. \begin_inset CommandInset ref
  5339. LatexCommand ref
  5340. reference "tab:Number-signif-promoters"
  5341. plural "false"
  5342. caps "false"
  5343. noprefix "false"
  5344. \end_inset
  5345. .
  5346. For all histone marks, evidence of differential modification between naïve
  5347. and memory samples was detected at every time point except day 14.
  5348. The day 14 convergence pattern is also present in the
  5349. \begin_inset Flex Glossary Term
  5350. status open
  5351. \begin_layout Plain Layout
  5352. RNA-seq
  5353. \end_layout
  5354. \end_inset
  5355. data (Figure
  5356. \begin_inset CommandInset ref
  5357. LatexCommand ref
  5358. reference "fig:RNA-PCA-group"
  5359. plural "false"
  5360. caps "false"
  5361. noprefix "false"
  5362. \end_inset
  5363. ), albeit in the 2nd and 3rd principal coordinates, indicating that it is
  5364. not the most dominant pattern driving gene expression.
  5365. Taken together, the data show that promoter histone methylation for these
  5366. 3 histone marks and RNA expression for naïve and memory cells are most
  5367. similar at day 14, the furthest time point after activation.
  5368. \begin_inset Flex Glossary Term
  5369. status open
  5370. \begin_layout Plain Layout
  5371. MOFA
  5372. \end_layout
  5373. \end_inset
  5374. was also able to capture this day 14 convergence pattern in
  5375. \begin_inset Flex Glossary Term
  5376. status open
  5377. \begin_layout Plain Layout
  5378. LF
  5379. \end_layout
  5380. \end_inset
  5381. 5 (Figure
  5382. \begin_inset CommandInset ref
  5383. LatexCommand ref
  5384. reference "fig:mofa-lf-scatter"
  5385. plural "false"
  5386. caps "false"
  5387. noprefix "false"
  5388. \end_inset
  5389. ), which accounts for shared variation across all 3 histone marks and the
  5390. \begin_inset Flex Glossary Term
  5391. status open
  5392. \begin_layout Plain Layout
  5393. RNA-seq
  5394. \end_layout
  5395. \end_inset
  5396. data, confirming that this convergence is a coordinated pattern across
  5397. all 4 data sets.
  5398. While this observation does not prove that the naïve cells have differentiated
  5399. into memory cells at Day 14, it is consistent with that hypothesis.
  5400. \end_layout
  5401. \begin_layout Standard
  5402. \begin_inset Float figure
  5403. placement p
  5404. wide false
  5405. sideways false
  5406. status open
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  5408. \align center
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  5410. wide false
  5411. sideways false
  5412. status open
  5413. \begin_layout Plain Layout
  5414. \align center
  5415. \begin_inset Graphics
  5416. filename graphics/CD4-csaw/ChIP-seq/H3K4me2-promoter-PCA-group-CROP.png
  5417. lyxscale 25
  5418. width 45col%
  5419. groupId pcoa-prom-subfig
  5420. \end_inset
  5421. \end_layout
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  5423. \begin_inset Caption Standard
  5424. \begin_layout Plain Layout
  5425. \begin_inset CommandInset label
  5426. LatexCommand label
  5427. name "fig:PCoA-H3K4me2-prom"
  5428. \end_inset
  5429. PCoA plot of H3K4me2 promoters, after subtracting surrogate variables.
  5430. \end_layout
  5431. \end_inset
  5432. \end_layout
  5433. \end_inset
  5434. \begin_inset space \hfill{}
  5435. \end_inset
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  5437. wide false
  5438. sideways false
  5439. status open
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  5441. \align center
  5442. \begin_inset Graphics
  5443. filename graphics/CD4-csaw/ChIP-seq/H3K4me3-promoter-PCA-group-CROP.png
  5444. lyxscale 25
  5445. width 45col%
  5446. groupId pcoa-prom-subfig
  5447. \end_inset
  5448. \end_layout
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  5452. \begin_inset CommandInset label
  5453. LatexCommand label
  5454. name "fig:PCoA-H3K4me3-prom"
  5455. \end_inset
  5456. PCoA plot of H3K4me3 promoters, after subtracting surrogate variables.
  5457. \end_layout
  5458. \end_inset
  5459. \end_layout
  5460. \end_inset
  5461. \end_layout
  5462. \begin_layout Plain Layout
  5463. \align center
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  5465. wide false
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  5467. status open
  5468. \begin_layout Plain Layout
  5469. \align center
  5470. \begin_inset Graphics
  5471. filename graphics/CD4-csaw/ChIP-seq/H3K27me3-promoter-PCA-group-CROP.png
  5472. lyxscale 25
  5473. width 45col%
  5474. groupId pcoa-prom-subfig
  5475. \end_inset
  5476. \end_layout
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  5479. \begin_layout Plain Layout
  5480. \begin_inset CommandInset label
  5481. LatexCommand label
  5482. name "fig:PCoA-H3K27me3-prom"
  5483. \end_inset
  5484. PCoA plot of H3K27me3 promoters, after subtracting surrogate variables.
  5485. \end_layout
  5486. \end_inset
  5487. \end_layout
  5488. \end_inset
  5489. \begin_inset space \hfill{}
  5490. \end_inset
  5491. \begin_inset Float figure
  5492. wide false
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  5494. status open
  5495. \begin_layout Plain Layout
  5496. \align center
  5497. \begin_inset Graphics
  5498. filename graphics/CD4-csaw/RNA-seq/PCA-final-23-CROP.png
  5499. lyxscale 25
  5500. width 45col%
  5501. groupId pcoa-prom-subfig
  5502. \end_inset
  5503. \end_layout
  5504. \begin_layout Plain Layout
  5505. \begin_inset Caption Standard
  5506. \begin_layout Plain Layout
  5507. \begin_inset CommandInset label
  5508. LatexCommand label
  5509. name "fig:RNA-PCA-group"
  5510. \end_inset
  5511. RNA-seq PCoA, after ComBat batch correction, showing principal coordinates
  5512. 2 and 3.
  5513. \end_layout
  5514. \end_inset
  5515. \end_layout
  5516. \end_inset
  5517. \end_layout
  5518. \begin_layout Plain Layout
  5519. \begin_inset Flex TODO Note (inline)
  5520. status open
  5521. \begin_layout Plain Layout
  5522. Figure font too small
  5523. \end_layout
  5524. \end_inset
  5525. \end_layout
  5526. \begin_layout Plain Layout
  5527. \begin_inset Caption Standard
  5528. \begin_layout Plain Layout
  5529. \begin_inset Argument 1
  5530. status collapsed
  5531. \begin_layout Plain Layout
  5532. PCoA plots for promoter ChIP-seq and expression RNA-seq data
  5533. \end_layout
  5534. \end_inset
  5535. \begin_inset CommandInset label
  5536. LatexCommand label
  5537. name "fig:PCoA-promoters"
  5538. \end_inset
  5539. \series bold
  5540. PCoA plots for promoter ChIP-seq and expression RNA-seq data.
  5541. \series default
  5542. Each point represents an individual sample.
  5543. Samples with the same combination of cell type and time point are encircled
  5544. with a shaded region to aid in visual identification of the sample groups.
  5545. Samples of the same cell type from the same donor are connected by lines
  5546. to indicate the
  5547. \begin_inset Quotes eld
  5548. \end_inset
  5549. trajectory
  5550. \begin_inset Quotes erd
  5551. \end_inset
  5552. of each donor's cells over time in PCoA space.
  5553. \end_layout
  5554. \end_inset
  5555. \end_layout
  5556. \end_inset
  5557. \end_layout
  5558. \begin_layout Standard
  5559. \begin_inset ERT
  5560. status open
  5561. \begin_layout Plain Layout
  5562. \backslash
  5563. afterpage{
  5564. \end_layout
  5565. \begin_layout Plain Layout
  5566. \backslash
  5567. begin{landscape}
  5568. \end_layout
  5569. \end_inset
  5570. \end_layout
  5571. \begin_layout Standard
  5572. \begin_inset Float table
  5573. wide false
  5574. sideways false
  5575. status collapsed
  5576. \begin_layout Plain Layout
  5577. \align center
  5578. \begin_inset Tabular
  5579. <lyxtabular version="3" rows="6" columns="7">
  5580. <features tabularvalignment="middle">
  5581. <column alignment="center" valignment="top">
  5582. <column alignment="center" valignment="top">
  5583. <column alignment="center" valignment="top">
  5584. <column alignment="center" valignment="top">
  5585. <column alignment="center" valignment="top">
  5586. <column alignment="center" valignment="top">
  5587. <column alignment="center" valignment="top">
  5588. <row>
  5589. <cell alignment="center" valignment="top" usebox="none">
  5590. \begin_inset Text
  5591. \begin_layout Plain Layout
  5592. \end_layout
  5593. \end_inset
  5594. </cell>
  5595. <cell multicolumn="1" alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  5596. \begin_inset Text
  5597. \begin_layout Plain Layout
  5598. Number of significant promoters
  5599. \end_layout
  5600. \end_inset
  5601. </cell>
  5602. <cell multicolumn="2" alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  5603. \begin_inset Text
  5604. \begin_layout Plain Layout
  5605. \end_layout
  5606. \end_inset
  5607. </cell>
  5608. <cell multicolumn="2" alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  5609. \begin_inset Text
  5610. \begin_layout Plain Layout
  5611. \end_layout
  5612. \end_inset
  5613. </cell>
  5614. <cell multicolumn="1" alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  5615. \begin_inset Text
  5616. \begin_layout Plain Layout
  5617. Est.
  5618. differentially modified promoters
  5619. \end_layout
  5620. \end_inset
  5621. </cell>
  5622. <cell multicolumn="2" alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  5623. \begin_inset Text
  5624. \begin_layout Plain Layout
  5625. \end_layout
  5626. \end_inset
  5627. </cell>
  5628. <cell multicolumn="2" alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  5629. \begin_inset Text
  5630. \begin_layout Plain Layout
  5631. \end_layout
  5632. \end_inset
  5633. </cell>
  5634. </row>
  5635. <row>
  5636. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  5637. \begin_inset Text
  5638. \begin_layout Plain Layout
  5639. Time Point
  5640. \end_layout
  5641. \end_inset
  5642. </cell>
  5643. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  5644. \begin_inset Text
  5645. \begin_layout Plain Layout
  5646. H3K4me2
  5647. \end_layout
  5648. \end_inset
  5649. </cell>
  5650. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  5651. \begin_inset Text
  5652. \begin_layout Plain Layout
  5653. H3K4me3
  5654. \end_layout
  5655. \end_inset
  5656. </cell>
  5657. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" rightline="true" usebox="none">
  5658. \begin_inset Text
  5659. \begin_layout Plain Layout
  5660. H3K27me3
  5661. \end_layout
  5662. \end_inset
  5663. </cell>
  5664. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  5665. \begin_inset Text
  5666. \begin_layout Plain Layout
  5667. H3K4me2
  5668. \end_layout
  5669. \end_inset
  5670. </cell>
  5671. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  5672. \begin_inset Text
  5673. \begin_layout Plain Layout
  5674. H3K4me3
  5675. \end_layout
  5676. \end_inset
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  5678. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" rightline="true" usebox="none">
  5679. \begin_inset Text
  5680. \begin_layout Plain Layout
  5681. H3K27me3
  5682. \end_layout
  5683. \end_inset
  5684. </cell>
  5685. </row>
  5686. <row>
  5687. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  5688. \begin_inset Text
  5689. \begin_layout Plain Layout
  5690. Day 0
  5691. \end_layout
  5692. \end_inset
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  5694. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  5695. \begin_inset Text
  5696. \begin_layout Plain Layout
  5697. 4553
  5698. \end_layout
  5699. \end_inset
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  5702. \begin_inset Text
  5703. \begin_layout Plain Layout
  5704. 927
  5705. \end_layout
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  5709. \begin_inset Text
  5710. \begin_layout Plain Layout
  5711. 6
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  5713. \end_inset
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  5715. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  5716. \begin_inset Text
  5717. \begin_layout Plain Layout
  5718. 9967
  5719. \end_layout
  5720. \end_inset
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  5722. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  5723. \begin_inset Text
  5724. \begin_layout Plain Layout
  5725. 4149
  5726. \end_layout
  5727. \end_inset
  5728. </cell>
  5729. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  5730. \begin_inset Text
  5731. \begin_layout Plain Layout
  5732. 2404
  5733. \end_layout
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  5737. <row>
  5738. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  5739. \begin_inset Text
  5740. \begin_layout Plain Layout
  5741. Day 1
  5742. \end_layout
  5743. \end_inset
  5744. </cell>
  5745. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  5746. \begin_inset Text
  5747. \begin_layout Plain Layout
  5748. 567
  5749. \end_layout
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  5753. \begin_inset Text
  5754. \begin_layout Plain Layout
  5755. 278
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  5758. </cell>
  5759. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  5760. \begin_inset Text
  5761. \begin_layout Plain Layout
  5762. 1570
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  5764. \end_inset
  5765. </cell>
  5766. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  5767. \begin_inset Text
  5768. \begin_layout Plain Layout
  5769. 4370
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  5774. \begin_inset Text
  5775. \begin_layout Plain Layout
  5776. 2145
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  5779. </cell>
  5780. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  5781. \begin_inset Text
  5782. \begin_layout Plain Layout
  5783. 6598
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  5788. <row>
  5789. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  5790. \begin_inset Text
  5791. \begin_layout Plain Layout
  5792. Day 5
  5793. \end_layout
  5794. \end_inset
  5795. </cell>
  5796. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  5797. \begin_inset Text
  5798. \begin_layout Plain Layout
  5799. 2313
  5800. \end_layout
  5801. \end_inset
  5802. </cell>
  5803. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  5804. \begin_inset Text
  5805. \begin_layout Plain Layout
  5806. 139
  5807. \end_layout
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  5809. </cell>
  5810. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  5811. \begin_inset Text
  5812. \begin_layout Plain Layout
  5813. 490
  5814. \end_layout
  5815. \end_inset
  5816. </cell>
  5817. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  5818. \begin_inset Text
  5819. \begin_layout Plain Layout
  5820. 9450
  5821. \end_layout
  5822. \end_inset
  5823. </cell>
  5824. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  5825. \begin_inset Text
  5826. \begin_layout Plain Layout
  5827. 1148
  5828. \end_layout
  5829. \end_inset
  5830. </cell>
  5831. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  5832. \begin_inset Text
  5833. \begin_layout Plain Layout
  5834. 4141
  5835. \end_layout
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  5837. </cell>
  5838. </row>
  5839. <row>
  5840. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  5841. \begin_inset Text
  5842. \begin_layout Plain Layout
  5843. Day 14
  5844. \end_layout
  5845. \end_inset
  5846. </cell>
  5847. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  5848. \begin_inset Text
  5849. \begin_layout Plain Layout
  5850. 0
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  5854. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
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  5857. 0
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  5862. \begin_inset Text
  5863. \begin_layout Plain Layout
  5864. 0
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  5867. </cell>
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  5869. \begin_inset Text
  5870. \begin_layout Plain Layout
  5871. 0
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  5874. </cell>
  5875. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  5876. \begin_inset Text
  5877. \begin_layout Plain Layout
  5878. 0
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  5881. </cell>
  5882. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" rightline="true" usebox="none">
  5883. \begin_inset Text
  5884. \begin_layout Plain Layout
  5885. 0
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  5887. \end_inset
  5888. </cell>
  5889. </row>
  5890. </lyxtabular>
  5891. \end_inset
  5892. \end_layout
  5893. \begin_layout Plain Layout
  5894. \begin_inset Caption Standard
  5895. \begin_layout Plain Layout
  5896. \begin_inset Argument 1
  5897. status collapsed
  5898. \begin_layout Plain Layout
  5899. Number of differentially modified promoters between naïve and memory cells
  5900. at each time point after activation.
  5901. \end_layout
  5902. \end_inset
  5903. \begin_inset CommandInset label
  5904. LatexCommand label
  5905. name "tab:Number-signif-promoters"
  5906. \end_inset
  5907. \series bold
  5908. Number of differentially modified promoters between naïve and memory cells
  5909. at each time point after activation.
  5910. \series default
  5911. This table shows both the number of differentially modified promoters detected
  5912. at a 10% FDR threshold (left half), and the total number of differentially
  5913. modified promoters estimated using the method of averaging local FDR estimates
  5914. \begin_inset CommandInset citation
  5915. LatexCommand cite
  5916. key "Phipson2013"
  5917. literal "false"
  5918. \end_inset
  5919. (right half).
  5920. \end_layout
  5921. \end_inset
  5922. \end_layout
  5923. \end_inset
  5924. \end_layout
  5925. \begin_layout Standard
  5926. \begin_inset ERT
  5927. status open
  5928. \begin_layout Plain Layout
  5929. \backslash
  5930. end{landscape}
  5931. \end_layout
  5932. \begin_layout Plain Layout
  5933. }
  5934. \end_layout
  5935. \end_inset
  5936. \end_layout
  5937. \begin_layout Subsection
  5938. Effect of H3K4me2 and H3K4me3 promoter coverage upstream vs downstream of
  5939. TSS
  5940. \end_layout
  5941. \begin_layout Standard
  5942. \begin_inset Flex TODO Note (inline)
  5943. status open
  5944. \begin_layout Plain Layout
  5945. Need a better section title, for this and the next one.
  5946. \end_layout
  5947. \end_inset
  5948. \end_layout
  5949. \begin_layout Standard
  5950. \begin_inset Flex TODO Note (inline)
  5951. status open
  5952. \begin_layout Plain Layout
  5953. Make sure use of coverage/abundance/whatever is consistent.
  5954. \end_layout
  5955. \end_inset
  5956. \end_layout
  5957. \begin_layout Standard
  5958. \begin_inset Flex TODO Note (inline)
  5959. status open
  5960. \begin_layout Plain Layout
  5961. For the figures in this section and the next, the group labels are arbitrary,
  5962. so if time allows, it would be good to manually reorder them in a logical
  5963. way, e.g.
  5964. most upstream to most downstream.
  5965. If this is done, make sure to update the text with the correct group labels.
  5966. \end_layout
  5967. \end_inset
  5968. \end_layout
  5969. \begin_layout Standard
  5970. To test whether the position of a histone mark relative to a gene's
  5971. \begin_inset Flex Glossary Term
  5972. status open
  5973. \begin_layout Plain Layout
  5974. TSS
  5975. \end_layout
  5976. \end_inset
  5977. was important, we looked at the
  5978. \begin_inset Quotes eld
  5979. \end_inset
  5980. landscape
  5981. \begin_inset Quotes erd
  5982. \end_inset
  5983. of
  5984. \begin_inset Flex Glossary Term
  5985. status open
  5986. \begin_layout Plain Layout
  5987. ChIP-seq
  5988. \end_layout
  5989. \end_inset
  5990. read coverage in naïve Day 0 samples within 5 kb of each gene's
  5991. \begin_inset Flex Glossary Term
  5992. status open
  5993. \begin_layout Plain Layout
  5994. TSS
  5995. \end_layout
  5996. \end_inset
  5997. by binning reads into 500-bp windows tiled across each promoter
  5998. \begin_inset Flex Glossary Term
  5999. status open
  6000. \begin_layout Plain Layout
  6001. logCPM
  6002. \end_layout
  6003. \end_inset
  6004. values were calculated for the bins in each promoter and then the average
  6005. \begin_inset Flex Glossary Term
  6006. status open
  6007. \begin_layout Plain Layout
  6008. logCPM
  6009. \end_layout
  6010. \end_inset
  6011. for each promoter's bins was normalized to zero, such that the values represent
  6012. coverage relative to other regions of the same promoter rather than being
  6013. proportional to absolute read count.
  6014. The promoters were then clustered based on the normalized bin abundances
  6015. using
  6016. \begin_inset Formula $k$
  6017. \end_inset
  6018. -means clustering with
  6019. \begin_inset Formula $K=6$
  6020. \end_inset
  6021. .
  6022. Different values of
  6023. \begin_inset Formula $K$
  6024. \end_inset
  6025. were also tested, but did not substantially change the interpretation of
  6026. the data.
  6027. \end_layout
  6028. \begin_layout Standard
  6029. For H3K4me2, plotting the average bin abundances for each cluster reveals
  6030. a simple pattern (Figure
  6031. \begin_inset CommandInset ref
  6032. LatexCommand ref
  6033. reference "fig:H3K4me2-neighborhood-clusters"
  6034. plural "false"
  6035. caps "false"
  6036. noprefix "false"
  6037. \end_inset
  6038. ): Cluster 5 represents a completely flat promoter coverage profile, likely
  6039. consisting of genes with no H3K4me2 methylation in the promoter.
  6040. All the other clusters represent a continuum of peak positions relative
  6041. to the
  6042. \begin_inset Flex Glossary Term
  6043. status open
  6044. \begin_layout Plain Layout
  6045. TSS
  6046. \end_layout
  6047. \end_inset
  6048. .
  6049. In order from most upstream to most downstream, they are Clusters 6, 4,
  6050. 3, 1, and 2.
  6051. There do not appear to be any clusters representing coverage patterns other
  6052. than lone peaks, such as coverage troughs or double peaks.
  6053. Next, all promoters were plotted in a
  6054. \begin_inset Flex Glossary Term
  6055. status open
  6056. \begin_layout Plain Layout
  6057. PCA
  6058. \end_layout
  6059. \end_inset
  6060. plot based on the same relative bin abundance data, and colored based on
  6061. cluster membership (Figure
  6062. \begin_inset CommandInset ref
  6063. LatexCommand ref
  6064. reference "fig:H3K4me2-neighborhood-pca"
  6065. plural "false"
  6066. caps "false"
  6067. noprefix "false"
  6068. \end_inset
  6069. ).
  6070. The
  6071. \begin_inset Flex Glossary Term
  6072. status open
  6073. \begin_layout Plain Layout
  6074. PCA
  6075. \end_layout
  6076. \end_inset
  6077. plot shows Cluster 5 (the
  6078. \begin_inset Quotes eld
  6079. \end_inset
  6080. no peak
  6081. \begin_inset Quotes erd
  6082. \end_inset
  6083. cluster) at the center, with the other clusters arranged in a counter-clockwise
  6084. arc around it in the order noted above, from most upstream peak to most
  6085. downstream.
  6086. Notably, the
  6087. \begin_inset Quotes eld
  6088. \end_inset
  6089. clusters
  6090. \begin_inset Quotes erd
  6091. \end_inset
  6092. form a single large
  6093. \begin_inset Quotes eld
  6094. \end_inset
  6095. cloud
  6096. \begin_inset Quotes erd
  6097. \end_inset
  6098. with no apparent separation between them, further supporting the conclusion
  6099. that these clusters represent an arbitrary partitioning of a continuous
  6100. distribution of promoter coverage landscapes.
  6101. While the clusters are a useful abstraction that aids in visualization,
  6102. they are ultimately not an accurate representation of the data.
  6103. The continuous nature of the distribution also explains why different values
  6104. of
  6105. \begin_inset Formula $K$
  6106. \end_inset
  6107. led to similar conclusions.
  6108. \end_layout
  6109. \begin_layout Standard
  6110. \begin_inset ERT
  6111. status open
  6112. \begin_layout Plain Layout
  6113. \backslash
  6114. afterpage{
  6115. \end_layout
  6116. \begin_layout Plain Layout
  6117. \backslash
  6118. begin{landscape}
  6119. \end_layout
  6120. \end_inset
  6121. \end_layout
  6122. \begin_layout Standard
  6123. \begin_inset Float figure
  6124. wide false
  6125. sideways false
  6126. status collapsed
  6127. \begin_layout Plain Layout
  6128. \align center
  6129. \begin_inset Float figure
  6130. wide false
  6131. sideways false
  6132. status open
  6133. \begin_layout Plain Layout
  6134. \align center
  6135. \begin_inset Graphics
  6136. filename graphics/CD4-csaw/ChIP-seq/H3K4me2-neighborhood-clusters-CROP.png
  6137. lyxscale 25
  6138. width 30col%
  6139. groupId covprof-subfig
  6140. \end_inset
  6141. \end_layout
  6142. \begin_layout Plain Layout
  6143. \begin_inset Caption Standard
  6144. \begin_layout Plain Layout
  6145. \series bold
  6146. \begin_inset CommandInset label
  6147. LatexCommand label
  6148. name "fig:H3K4me2-neighborhood-clusters"
  6149. \end_inset
  6150. Average relative coverage for each bin in each cluster.
  6151. \end_layout
  6152. \end_inset
  6153. \end_layout
  6154. \end_inset
  6155. \begin_inset space \hfill{}
  6156. \end_inset
  6157. \begin_inset Float figure
  6158. wide false
  6159. sideways false
  6160. status open
  6161. \begin_layout Plain Layout
  6162. \align center
  6163. \begin_inset Graphics
  6164. filename graphics/CD4-csaw/ChIP-seq/H3K4me2-neighborhood-PCA-CROP.png
  6165. lyxscale 25
  6166. width 30col%
  6167. groupId covprof-subfig
  6168. \end_inset
  6169. \end_layout
  6170. \begin_layout Plain Layout
  6171. \begin_inset Caption Standard
  6172. \begin_layout Plain Layout
  6173. \begin_inset CommandInset label
  6174. LatexCommand label
  6175. name "fig:H3K4me2-neighborhood-pca"
  6176. \end_inset
  6177. PCA of relative coverage depth, colored by K-means cluster membership.
  6178. \end_layout
  6179. \end_inset
  6180. \end_layout
  6181. \end_inset
  6182. \begin_inset space \hfill{}
  6183. \end_inset
  6184. \begin_inset Float figure
  6185. wide false
  6186. sideways false
  6187. status open
  6188. \begin_layout Plain Layout
  6189. \align center
  6190. \begin_inset Graphics
  6191. filename graphics/CD4-csaw/ChIP-seq/H3K4me2-neighborhood-expression-CROP.png
  6192. lyxscale 25
  6193. width 30col%
  6194. groupId covprof-subfig
  6195. \end_inset
  6196. \end_layout
  6197. \begin_layout Plain Layout
  6198. \begin_inset Caption Standard
  6199. \begin_layout Plain Layout
  6200. \begin_inset CommandInset label
  6201. LatexCommand label
  6202. name "fig:H3K4me2-neighborhood-expression"
  6203. \end_inset
  6204. Gene expression grouped by promoter coverage clusters.
  6205. \end_layout
  6206. \end_inset
  6207. \end_layout
  6208. \end_inset
  6209. \end_layout
  6210. \begin_layout Plain Layout
  6211. \begin_inset Flex TODO Note (inline)
  6212. status open
  6213. \begin_layout Plain Layout
  6214. Figure font too small
  6215. \end_layout
  6216. \end_inset
  6217. \end_layout
  6218. \begin_layout Plain Layout
  6219. \begin_inset Caption Standard
  6220. \begin_layout Plain Layout
  6221. \begin_inset Argument 1
  6222. status collapsed
  6223. \begin_layout Plain Layout
  6224. K-means clustering of promoter H3K4me2 relative coverage depth in naïve
  6225. day 0 samples.
  6226. \end_layout
  6227. \end_inset
  6228. \begin_inset CommandInset label
  6229. LatexCommand label
  6230. name "fig:H3K4me2-neighborhood"
  6231. \end_inset
  6232. \series bold
  6233. K-means clustering of promoter H3K4me2 relative coverage depth in naïve
  6234. day 0 samples.
  6235. \series default
  6236. H3K4me2 ChIP-seq reads were binned into 500-bp windows tiled across each
  6237. promoter from 5
  6238. \begin_inset space ~
  6239. \end_inset
  6240. kbp upstream to 5
  6241. \begin_inset space ~
  6242. \end_inset
  6243. kbp downstream, and the logCPM values were normalized within each promoter
  6244. to an average of 0, yielding relative coverage depths.
  6245. These were then grouped using K-means clustering with
  6246. \begin_inset Formula $K=6$
  6247. \end_inset
  6248. ,
  6249. \series bold
  6250. \series default
  6251. and the average bin values were plotted for each cluster (a).
  6252. The
  6253. \begin_inset Formula $x$
  6254. \end_inset
  6255. -axis is the genomic coordinate of each bin relative to the the transcription
  6256. start site, and the
  6257. \begin_inset Formula $y$
  6258. \end_inset
  6259. -axis is the mean relative coverage depth of that bin across all promoters
  6260. in the cluster.
  6261. Each line represents the average
  6262. \begin_inset Quotes eld
  6263. \end_inset
  6264. shape
  6265. \begin_inset Quotes erd
  6266. \end_inset
  6267. of the promoter coverage for promoters in that cluster.
  6268. PCA was performed on the same data, and the first two PCs were plotted,
  6269. coloring each point by its K-means cluster identity (b).
  6270. For each cluster, the distribution of gene expression values was plotted
  6271. (c).
  6272. \end_layout
  6273. \end_inset
  6274. \end_layout
  6275. \end_inset
  6276. \end_layout
  6277. \begin_layout Standard
  6278. \begin_inset ERT
  6279. status open
  6280. \begin_layout Plain Layout
  6281. \backslash
  6282. end{landscape}
  6283. \end_layout
  6284. \begin_layout Plain Layout
  6285. }
  6286. \end_layout
  6287. \end_inset
  6288. \end_layout
  6289. \begin_layout Standard
  6290. \begin_inset Flex TODO Note (inline)
  6291. status open
  6292. \begin_layout Plain Layout
  6293. Should have a table of p-values on difference of means between Cluster 5
  6294. and the others.
  6295. \end_layout
  6296. \end_inset
  6297. \end_layout
  6298. \begin_layout Standard
  6299. To investigate the association between relative peak position and gene expressio
  6300. n, we plotted the Naïve Day 0 expression for the genes in each cluster (Figure
  6301. \begin_inset CommandInset ref
  6302. LatexCommand ref
  6303. reference "fig:H3K4me2-neighborhood-expression"
  6304. plural "false"
  6305. caps "false"
  6306. noprefix "false"
  6307. \end_inset
  6308. ).
  6309. Most genes in Cluster 5, the
  6310. \begin_inset Quotes eld
  6311. \end_inset
  6312. no peak
  6313. \begin_inset Quotes erd
  6314. \end_inset
  6315. cluster, have low expression values.
  6316. Taking this as the
  6317. \begin_inset Quotes eld
  6318. \end_inset
  6319. baseline
  6320. \begin_inset Quotes erd
  6321. \end_inset
  6322. distribution when no H3K4me2 methylation is present, we can compare the
  6323. other clusters' distributions to determine which peak positions are associated
  6324. with elevated expression.
  6325. As might be expected, the 3 clusters representing peaks closest to the
  6326. \begin_inset Flex Glossary Term
  6327. status open
  6328. \begin_layout Plain Layout
  6329. TSS
  6330. \end_layout
  6331. \end_inset
  6332. , Clusters 1, 3, and 4, show the highest average expression distributions.
  6333. Specifically, these clusters all have their highest
  6334. \begin_inset Flex Glossary Term
  6335. status open
  6336. \begin_layout Plain Layout
  6337. ChIP-seq
  6338. \end_layout
  6339. \end_inset
  6340. abundance within 1kb of the
  6341. \begin_inset Flex Glossary Term
  6342. status open
  6343. \begin_layout Plain Layout
  6344. TSS
  6345. \end_layout
  6346. \end_inset
  6347. , consistent with the previously determined promoter radius.
  6348. In contrast, cluster 6, which represents peaks several kb upstream of the
  6349. \begin_inset Flex Glossary Term
  6350. status open
  6351. \begin_layout Plain Layout
  6352. TSS
  6353. \end_layout
  6354. \end_inset
  6355. , shows a slightly higher average expression than baseline, while Cluster
  6356. 2, which represents peaks several kb downstream, doesn't appear to show
  6357. any appreciable difference.
  6358. Interestingly, the cluster with the highest average expression is Cluster
  6359. 1, which represents peaks about 1 kb downstream of the
  6360. \begin_inset Flex Glossary Term
  6361. status open
  6362. \begin_layout Plain Layout
  6363. TSS
  6364. \end_layout
  6365. \end_inset
  6366. , rather than Cluster 3, which represents peaks centered directly at the
  6367. \begin_inset Flex Glossary Term
  6368. status open
  6369. \begin_layout Plain Layout
  6370. TSS
  6371. \end_layout
  6372. \end_inset
  6373. .
  6374. This suggests that conceptualizing the promoter as a region centered on
  6375. the
  6376. \begin_inset Flex Glossary Term
  6377. status open
  6378. \begin_layout Plain Layout
  6379. TSS
  6380. \end_layout
  6381. \end_inset
  6382. with a certain
  6383. \begin_inset Quotes eld
  6384. \end_inset
  6385. radius
  6386. \begin_inset Quotes erd
  6387. \end_inset
  6388. may be an oversimplification – a peak that is a specific distance from
  6389. the
  6390. \begin_inset Flex Glossary Term
  6391. status open
  6392. \begin_layout Plain Layout
  6393. TSS
  6394. \end_layout
  6395. \end_inset
  6396. may have a different degree of influence depending on whether it is upstream
  6397. or downstream of the
  6398. \begin_inset Flex Glossary Term
  6399. status open
  6400. \begin_layout Plain Layout
  6401. TSS
  6402. \end_layout
  6403. \end_inset
  6404. .
  6405. \end_layout
  6406. \begin_layout Standard
  6407. All observations described above for H3K4me2
  6408. \begin_inset Flex Glossary Term
  6409. status open
  6410. \begin_layout Plain Layout
  6411. ChIP-seq
  6412. \end_layout
  6413. \end_inset
  6414. also appear to hold for H3K4me3 as well (Figure
  6415. \begin_inset CommandInset ref
  6416. LatexCommand ref
  6417. reference "fig:H3K4me3-neighborhood"
  6418. plural "false"
  6419. caps "false"
  6420. noprefix "false"
  6421. \end_inset
  6422. ).
  6423. This is expected, since there is a high correlation between the positions
  6424. where both histone marks occur.
  6425. \end_layout
  6426. \begin_layout Standard
  6427. \begin_inset ERT
  6428. status open
  6429. \begin_layout Plain Layout
  6430. \backslash
  6431. afterpage{
  6432. \end_layout
  6433. \begin_layout Plain Layout
  6434. \backslash
  6435. begin{landscape}
  6436. \end_layout
  6437. \end_inset
  6438. \end_layout
  6439. \begin_layout Standard
  6440. \begin_inset Float figure
  6441. wide false
  6442. sideways false
  6443. status open
  6444. \begin_layout Plain Layout
  6445. \align center
  6446. \begin_inset Float figure
  6447. wide false
  6448. sideways false
  6449. status open
  6450. \begin_layout Plain Layout
  6451. \align center
  6452. \begin_inset Graphics
  6453. filename graphics/CD4-csaw/ChIP-seq/H3K4me3-neighborhood-clusters-CROP.png
  6454. lyxscale 25
  6455. width 30col%
  6456. groupId covprof-subfig
  6457. \end_inset
  6458. \end_layout
  6459. \begin_layout Plain Layout
  6460. \begin_inset Caption Standard
  6461. \begin_layout Plain Layout
  6462. \begin_inset CommandInset label
  6463. LatexCommand label
  6464. name "fig:H3K4me3-neighborhood-clusters"
  6465. \end_inset
  6466. Average relative coverage for each bin in each cluster.
  6467. \end_layout
  6468. \end_inset
  6469. \end_layout
  6470. \end_inset
  6471. \begin_inset space \hfill{}
  6472. \end_inset
  6473. \begin_inset Float figure
  6474. wide false
  6475. sideways false
  6476. status open
  6477. \begin_layout Plain Layout
  6478. \align center
  6479. \begin_inset Graphics
  6480. filename graphics/CD4-csaw/ChIP-seq/H3K4me3-neighborhood-PCA-CROP.png
  6481. lyxscale 25
  6482. width 30col%
  6483. groupId covprof-subfig
  6484. \end_inset
  6485. \end_layout
  6486. \begin_layout Plain Layout
  6487. \begin_inset Caption Standard
  6488. \begin_layout Plain Layout
  6489. \begin_inset CommandInset label
  6490. LatexCommand label
  6491. name "fig:H3K4me3-neighborhood-pca"
  6492. \end_inset
  6493. PCA of relative coverage depth, colored by K-means cluster membership.
  6494. \end_layout
  6495. \end_inset
  6496. \end_layout
  6497. \end_inset
  6498. \begin_inset space \hfill{}
  6499. \end_inset
  6500. \begin_inset Float figure
  6501. wide false
  6502. sideways false
  6503. status open
  6504. \begin_layout Plain Layout
  6505. \align center
  6506. \begin_inset Graphics
  6507. filename graphics/CD4-csaw/ChIP-seq/H3K4me3-neighborhood-expression-CROP.png
  6508. lyxscale 25
  6509. width 30col%
  6510. groupId covprof-subfig
  6511. \end_inset
  6512. \end_layout
  6513. \begin_layout Plain Layout
  6514. \begin_inset Caption Standard
  6515. \begin_layout Plain Layout
  6516. \begin_inset CommandInset label
  6517. LatexCommand label
  6518. name "fig:H3K4me3-neighborhood-expression"
  6519. \end_inset
  6520. Gene expression grouped by promoter coverage clusters.
  6521. \end_layout
  6522. \end_inset
  6523. \end_layout
  6524. \end_inset
  6525. \end_layout
  6526. \begin_layout Plain Layout
  6527. \begin_inset Caption Standard
  6528. \begin_layout Plain Layout
  6529. \begin_inset Argument 1
  6530. status collapsed
  6531. \begin_layout Plain Layout
  6532. K-means clustering of promoter H3K4me3 relative coverage depth in naïve
  6533. day 0 samples.
  6534. \end_layout
  6535. \end_inset
  6536. \begin_inset CommandInset label
  6537. LatexCommand label
  6538. name "fig:H3K4me3-neighborhood"
  6539. \end_inset
  6540. \series bold
  6541. K-means clustering of promoter H3K4me3 relative coverage depth in naïve
  6542. day 0 samples.
  6543. \series default
  6544. H3K4me3 ChIP-seq reads were binned into 500-bp windows tiled across each
  6545. promoter from 5
  6546. \begin_inset space ~
  6547. \end_inset
  6548. kbp upstream to 5
  6549. \begin_inset space ~
  6550. \end_inset
  6551. kbp downstream, and the logCPM values were normalized within each promoter
  6552. to an average of 0, yielding relative coverage depths.
  6553. These were then grouped using K-means clustering with
  6554. \begin_inset Formula $K=6$
  6555. \end_inset
  6556. ,
  6557. \series bold
  6558. \series default
  6559. and the average bin values were plotted for each cluster (a).
  6560. The
  6561. \begin_inset Formula $x$
  6562. \end_inset
  6563. -axis is the genomic coordinate of each bin relative to the the transcription
  6564. start site, and the
  6565. \begin_inset Formula $y$
  6566. \end_inset
  6567. -axis is the mean relative coverage depth of that bin across all promoters
  6568. in the cluster.
  6569. Each line represents the average
  6570. \begin_inset Quotes eld
  6571. \end_inset
  6572. shape
  6573. \begin_inset Quotes erd
  6574. \end_inset
  6575. of the promoter coverage for promoters in that cluster.
  6576. PCA was performed on the same data, and the first two PCs were plotted,
  6577. coloring each point by its K-means cluster identity (b).
  6578. For each cluster, the distribution of gene expression values was plotted
  6579. (c).
  6580. \end_layout
  6581. \end_inset
  6582. \end_layout
  6583. \end_inset
  6584. \end_layout
  6585. \begin_layout Standard
  6586. \begin_inset ERT
  6587. status open
  6588. \begin_layout Plain Layout
  6589. \backslash
  6590. end{landscape}
  6591. \end_layout
  6592. \begin_layout Plain Layout
  6593. }
  6594. \end_layout
  6595. \end_inset
  6596. \end_layout
  6597. \begin_layout Subsection
  6598. Promoter coverage H3K27me3
  6599. \end_layout
  6600. \begin_layout Standard
  6601. Unlike both H3K4 marks, whose main patterns of variation appear directly
  6602. related to the size and position of a single peak within the promoter,
  6603. the patterns of H3K27me3 methylation in promoters are more complex (Figure
  6604. \begin_inset CommandInset ref
  6605. LatexCommand ref
  6606. reference "fig:H3K27me3-neighborhood"
  6607. plural "false"
  6608. caps "false"
  6609. noprefix "false"
  6610. \end_inset
  6611. ).
  6612. Once again looking at the relative coverage in a 500-bp wide bins in a
  6613. 5kb radius around each
  6614. \begin_inset Flex Glossary Term
  6615. status open
  6616. \begin_layout Plain Layout
  6617. TSS
  6618. \end_layout
  6619. \end_inset
  6620. , promoters were clustered based on the normalized relative coverage values
  6621. in each bin using
  6622. \begin_inset Formula $k$
  6623. \end_inset
  6624. -means clustering with
  6625. \begin_inset Formula $K=6$
  6626. \end_inset
  6627. (Figure
  6628. \begin_inset CommandInset ref
  6629. LatexCommand ref
  6630. reference "fig:H3K27me3-neighborhood-clusters"
  6631. plural "false"
  6632. caps "false"
  6633. noprefix "false"
  6634. \end_inset
  6635. ).
  6636. This time, 3
  6637. \begin_inset Quotes eld
  6638. \end_inset
  6639. axes
  6640. \begin_inset Quotes erd
  6641. \end_inset
  6642. of variation can be observed, each represented by 2 clusters with opposing
  6643. patterns.
  6644. The first axis is greater upstream coverage (Cluster 1) vs.
  6645. greater downstream coverage (Cluster 3); the second axis is the coverage
  6646. at the
  6647. \begin_inset Flex Glossary Term
  6648. status open
  6649. \begin_layout Plain Layout
  6650. TSS
  6651. \end_layout
  6652. \end_inset
  6653. itself: peak (Cluster 4) or trough (Cluster 2); lastly, the third axis
  6654. represents a trough upstream of the
  6655. \begin_inset Flex Glossary Term
  6656. status open
  6657. \begin_layout Plain Layout
  6658. TSS
  6659. \end_layout
  6660. \end_inset
  6661. (Cluster 5) vs.
  6662. downstream of the
  6663. \begin_inset Flex Glossary Term
  6664. status open
  6665. \begin_layout Plain Layout
  6666. TSS
  6667. \end_layout
  6668. \end_inset
  6669. (Cluster 6).
  6670. Referring to these opposing pairs of clusters as axes of variation is justified
  6671. , because they correspond precisely to the first 3
  6672. \begin_inset Flex Glossary Term (pl)
  6673. status open
  6674. \begin_layout Plain Layout
  6675. PC
  6676. \end_layout
  6677. \end_inset
  6678. in the
  6679. \begin_inset Flex Glossary Term
  6680. status open
  6681. \begin_layout Plain Layout
  6682. PCA
  6683. \end_layout
  6684. \end_inset
  6685. plot of the relative coverage values (Figure
  6686. \begin_inset CommandInset ref
  6687. LatexCommand ref
  6688. reference "fig:H3K27me3-neighborhood-pca"
  6689. plural "false"
  6690. caps "false"
  6691. noprefix "false"
  6692. \end_inset
  6693. ).
  6694. The
  6695. \begin_inset Flex Glossary Term
  6696. status open
  6697. \begin_layout Plain Layout
  6698. PCA
  6699. \end_layout
  6700. \end_inset
  6701. plot reveals that as in the case of H3K4me2, all the
  6702. \begin_inset Quotes eld
  6703. \end_inset
  6704. clusters
  6705. \begin_inset Quotes erd
  6706. \end_inset
  6707. are really just sections of a single connected cloud rather than discrete
  6708. clusters.
  6709. The cloud is approximately ellipsoid-shaped, with each PC being an axis
  6710. of the ellipse, and each cluster consisting of a pyramidal section of the
  6711. ellipsoid.
  6712. \end_layout
  6713. \begin_layout Standard
  6714. \begin_inset ERT
  6715. status open
  6716. \begin_layout Plain Layout
  6717. \backslash
  6718. afterpage{
  6719. \end_layout
  6720. \begin_layout Plain Layout
  6721. \backslash
  6722. begin{landscape}
  6723. \end_layout
  6724. \end_inset
  6725. \end_layout
  6726. \begin_layout Standard
  6727. \begin_inset Float figure
  6728. wide false
  6729. sideways false
  6730. status collapsed
  6731. \begin_layout Plain Layout
  6732. \align center
  6733. \begin_inset Float figure
  6734. wide false
  6735. sideways false
  6736. status open
  6737. \begin_layout Plain Layout
  6738. \align center
  6739. \begin_inset Graphics
  6740. filename graphics/CD4-csaw/ChIP-seq/H3K27me3-neighborhood-clusters-CROP.png
  6741. lyxscale 25
  6742. width 30col%
  6743. groupId covprof-subfig
  6744. \end_inset
  6745. \end_layout
  6746. \begin_layout Plain Layout
  6747. \begin_inset Caption Standard
  6748. \begin_layout Plain Layout
  6749. \begin_inset CommandInset label
  6750. LatexCommand label
  6751. name "fig:H3K27me3-neighborhood-clusters"
  6752. \end_inset
  6753. Average relative coverage for each bin in each cluster.
  6754. \end_layout
  6755. \end_inset
  6756. \end_layout
  6757. \end_inset
  6758. \begin_inset space \hfill{}
  6759. \end_inset
  6760. \begin_inset Float figure
  6761. wide false
  6762. sideways false
  6763. status open
  6764. \begin_layout Plain Layout
  6765. \align center
  6766. \begin_inset Graphics
  6767. filename graphics/CD4-csaw/ChIP-seq/H3K27me3-neighborhood-PCA-CROP.png
  6768. lyxscale 25
  6769. width 30col%
  6770. groupId covprof-subfig
  6771. \end_inset
  6772. \end_layout
  6773. \begin_layout Plain Layout
  6774. \begin_inset Caption Standard
  6775. \begin_layout Plain Layout
  6776. \begin_inset CommandInset label
  6777. LatexCommand label
  6778. name "fig:H3K27me3-neighborhood-pca"
  6779. \end_inset
  6780. PCA of relative coverage depth, colored by K-means cluster membership.
  6781. (Note: Cluster 6 is hidden behind all the other clusters.)
  6782. \end_layout
  6783. \end_inset
  6784. \end_layout
  6785. \end_inset
  6786. \begin_inset space \hfill{}
  6787. \end_inset
  6788. \begin_inset Float figure
  6789. wide false
  6790. sideways false
  6791. status open
  6792. \begin_layout Plain Layout
  6793. \align center
  6794. \begin_inset Graphics
  6795. filename graphics/CD4-csaw/ChIP-seq/H3K27me3-neighborhood-expression-CROP.png
  6796. lyxscale 25
  6797. width 30col%
  6798. groupId covprof-subfig
  6799. \end_inset
  6800. \end_layout
  6801. \begin_layout Plain Layout
  6802. \begin_inset Caption Standard
  6803. \begin_layout Plain Layout
  6804. \begin_inset CommandInset label
  6805. LatexCommand label
  6806. name "fig:H3K27me3-neighborhood-expression"
  6807. \end_inset
  6808. Gene expression grouped by promoter coverage clusters.
  6809. \end_layout
  6810. \end_inset
  6811. \end_layout
  6812. \end_inset
  6813. \end_layout
  6814. \begin_layout Plain Layout
  6815. \begin_inset Flex TODO Note (inline)
  6816. status open
  6817. \begin_layout Plain Layout
  6818. Repeated figure legends are kind of an issue here.
  6819. What to do?
  6820. \end_layout
  6821. \end_inset
  6822. \end_layout
  6823. \begin_layout Plain Layout
  6824. \begin_inset Caption Standard
  6825. \begin_layout Plain Layout
  6826. \begin_inset Argument 1
  6827. status collapsed
  6828. \begin_layout Plain Layout
  6829. K-means clustering of promoter H3K27me3 relative coverage depth in naïve
  6830. day 0 samples.
  6831. \end_layout
  6832. \end_inset
  6833. \begin_inset CommandInset label
  6834. LatexCommand label
  6835. name "fig:H3K27me3-neighborhood"
  6836. \end_inset
  6837. \series bold
  6838. K-means clustering of promoter H3K27me3 relative coverage depth in naïve
  6839. day 0 samples.
  6840. \series default
  6841. H3K27me3 ChIP-seq reads were binned into 500-bp windows tiled across each
  6842. promoter from 5
  6843. \begin_inset space ~
  6844. \end_inset
  6845. kbp upstream to 5
  6846. \begin_inset space ~
  6847. \end_inset
  6848. kbp downstream, and the logCPM values were normalized within each promoter
  6849. to an average of 0, yielding relative coverage depths.
  6850. These were then grouped using
  6851. \begin_inset Formula $k$
  6852. \end_inset
  6853. -means clustering with
  6854. \begin_inset Formula $K=6$
  6855. \end_inset
  6856. ,
  6857. \series bold
  6858. \series default
  6859. and the average bin values were plotted for each cluster (a).
  6860. The
  6861. \begin_inset Formula $x$
  6862. \end_inset
  6863. -axis is the genomic coordinate of each bin relative to the the transcription
  6864. start site, and the
  6865. \begin_inset Formula $y$
  6866. \end_inset
  6867. -axis is the mean relative coverage depth of that bin across all promoters
  6868. in the cluster.
  6869. Each line represents the average
  6870. \begin_inset Quotes eld
  6871. \end_inset
  6872. shape
  6873. \begin_inset Quotes erd
  6874. \end_inset
  6875. of the promoter coverage for promoters in that cluster.
  6876. PCA was performed on the same data, and the first two PCs were plotted,
  6877. coloring each point by its K-means cluster identity (b).
  6878. For each cluster, the distribution of gene expression values was plotted
  6879. (c).
  6880. \end_layout
  6881. \end_inset
  6882. \end_layout
  6883. \end_inset
  6884. \end_layout
  6885. \begin_layout Standard
  6886. \begin_inset ERT
  6887. status open
  6888. \begin_layout Plain Layout
  6889. \backslash
  6890. end{landscape}
  6891. \end_layout
  6892. \begin_layout Plain Layout
  6893. }
  6894. \end_layout
  6895. \end_inset
  6896. \end_layout
  6897. \begin_layout Standard
  6898. In Figure
  6899. \begin_inset CommandInset ref
  6900. LatexCommand ref
  6901. reference "fig:H3K27me3-neighborhood-expression"
  6902. plural "false"
  6903. caps "false"
  6904. noprefix "false"
  6905. \end_inset
  6906. , we can see that Clusters 1 and 2 are the only clusters with higher gene
  6907. expression than the others.
  6908. For Cluster 2, this is expected, since this cluster represents genes with
  6909. depletion of H3K27me3 near the promoter.
  6910. Hence, elevated expression in cluster 2 is consistent with the conventional
  6911. view of H3K27me3 as a deactivating mark.
  6912. However, Cluster 1, the cluster with the most elevated gene expression,
  6913. represents genes with elevated coverage upstream of the
  6914. \begin_inset Flex Glossary Term
  6915. status open
  6916. \begin_layout Plain Layout
  6917. TSS
  6918. \end_layout
  6919. \end_inset
  6920. , or equivalently, decreased coverage downstream, inside the gene body.
  6921. The opposite pattern, in which H3K27me3 is more abundant within the gene
  6922. body and less abundance in the upstream promoter region, does not show
  6923. any elevation in gene expression.
  6924. As with H3K4me2, this shows that the location of H3K27 trimethylation relative
  6925. to the
  6926. \begin_inset Flex Glossary Term
  6927. status open
  6928. \begin_layout Plain Layout
  6929. TSS
  6930. \end_layout
  6931. \end_inset
  6932. is potentially an important factor beyond simple proximity.
  6933. \end_layout
  6934. \begin_layout Standard
  6935. \begin_inset Flex TODO Note (inline)
  6936. status open
  6937. \begin_layout Plain Layout
  6938. Show the figures where the negative result ended this line of inquiry.
  6939. I need to debug some errors resulting from an R upgrade to do this.
  6940. \end_layout
  6941. \end_inset
  6942. \end_layout
  6943. \begin_layout Subsection
  6944. Defined pattern analysis
  6945. \end_layout
  6946. \begin_layout Standard
  6947. \begin_inset Flex TODO Note (inline)
  6948. status open
  6949. \begin_layout Plain Layout
  6950. This was where I defined interesting expression patterns and then looked
  6951. at initial relative promoter coverage for each expression pattern.
  6952. Negative result.
  6953. I forgot about this until recently.
  6954. Worth including? Remember to also write methods.
  6955. \end_layout
  6956. \end_inset
  6957. \end_layout
  6958. \begin_layout Subsection
  6959. Promoter CpG islands?
  6960. \end_layout
  6961. \begin_layout Standard
  6962. \begin_inset Flex TODO Note (inline)
  6963. status collapsed
  6964. \begin_layout Plain Layout
  6965. I forgot until recently about the work I did on this.
  6966. Worth including? Remember to also write methods.
  6967. \end_layout
  6968. \end_inset
  6969. \end_layout
  6970. \begin_layout Section
  6971. Discussion
  6972. \end_layout
  6973. \begin_layout Standard
  6974. \begin_inset Flex TODO Note (inline)
  6975. status open
  6976. \begin_layout Plain Layout
  6977. Write better section headers
  6978. \end_layout
  6979. \end_inset
  6980. \end_layout
  6981. \begin_layout Subsection
  6982. Effective promoter radius
  6983. \end_layout
  6984. \begin_layout Standard
  6985. Figure
  6986. \begin_inset CommandInset ref
  6987. LatexCommand ref
  6988. reference "fig:near-promoter-peak-enrich"
  6989. plural "false"
  6990. caps "false"
  6991. noprefix "false"
  6992. \end_inset
  6993. shows that H3K4me2, H3K4me3, and H3K27me3 are all enriched near promoters,
  6994. relative to the rest of the genome, consistent with their conventionally
  6995. understood role in regulating gene transcription.
  6996. Interestingly, the radius within this enrichment occurs is not the same
  6997. for each histone mark.
  6998. H3K4me2 and H3K4me3 are enriched within a 1
  6999. \begin_inset space \thinspace{}
  7000. \end_inset
  7001. kb radius, while H3K27me3 is enriched within 2.5
  7002. \begin_inset space \thinspace{}
  7003. \end_inset
  7004. kb.
  7005. Notably, the determined promoter radius was consistent across all experimental
  7006. conditions, varying only between different histone marks.
  7007. This suggests that the conventional
  7008. \begin_inset Quotes eld
  7009. \end_inset
  7010. one size fits all
  7011. \begin_inset Quotes erd
  7012. \end_inset
  7013. approach of defining a single promoter region for each gene (or each
  7014. \begin_inset Flex Glossary Term
  7015. status open
  7016. \begin_layout Plain Layout
  7017. TSS
  7018. \end_layout
  7019. \end_inset
  7020. ) and using that same promoter region for analyzing all types of genomic
  7021. data within an experiment may not be appropriate, and a better approach
  7022. may be to use a separate promoter radius for each kind of data, with each
  7023. radius being derived from the data itself.
  7024. Furthermore, the apparent asymmetry of upstream and downstream promoter
  7025. histone modification with respect to gene expression, seen in Figures
  7026. \begin_inset CommandInset ref
  7027. LatexCommand ref
  7028. reference "fig:H3K4me2-neighborhood"
  7029. plural "false"
  7030. caps "false"
  7031. noprefix "false"
  7032. \end_inset
  7033. ,
  7034. \begin_inset CommandInset ref
  7035. LatexCommand ref
  7036. reference "fig:H3K4me3-neighborhood"
  7037. plural "false"
  7038. caps "false"
  7039. noprefix "false"
  7040. \end_inset
  7041. , and
  7042. \begin_inset CommandInset ref
  7043. LatexCommand ref
  7044. reference "fig:H3K27me3-neighborhood"
  7045. plural "false"
  7046. caps "false"
  7047. noprefix "false"
  7048. \end_inset
  7049. , shows that even the concept of a promoter
  7050. \begin_inset Quotes eld
  7051. \end_inset
  7052. radius
  7053. \begin_inset Quotes erd
  7054. \end_inset
  7055. is likely an oversimplification.
  7056. At a minimum, nearby enrichment of peaks should be evaluated separately
  7057. for both upstream and downstream peaks, and an appropriate
  7058. \begin_inset Quotes eld
  7059. \end_inset
  7060. radius
  7061. \begin_inset Quotes erd
  7062. \end_inset
  7063. should be selected for each direction.
  7064. \end_layout
  7065. \begin_layout Standard
  7066. Figures
  7067. \begin_inset CommandInset ref
  7068. LatexCommand ref
  7069. reference "fig:H3K4me2-neighborhood"
  7070. plural "false"
  7071. caps "false"
  7072. noprefix "false"
  7073. \end_inset
  7074. and
  7075. \begin_inset CommandInset ref
  7076. LatexCommand ref
  7077. reference "fig:H3K4me3-neighborhood"
  7078. plural "false"
  7079. caps "false"
  7080. noprefix "false"
  7081. \end_inset
  7082. show that the determined promoter radius of 1
  7083. \begin_inset space ~
  7084. \end_inset
  7085. kb is approximately consistent with the distance from the
  7086. \begin_inset Flex Glossary Term
  7087. status open
  7088. \begin_layout Plain Layout
  7089. TSS
  7090. \end_layout
  7091. \end_inset
  7092. at which enrichment of H3K4 methylation correlates with increased expression,
  7093. showing that this radius, which was determined by a simple analysis of
  7094. measuring the distance from each
  7095. \begin_inset Flex Glossary Term
  7096. status open
  7097. \begin_layout Plain Layout
  7098. TSS
  7099. \end_layout
  7100. \end_inset
  7101. to the nearest peak, also has functional significance.
  7102. For H3K27me3, the correlation between histone modification near the promoter
  7103. and gene expression is more complex, involving non-peak variations such
  7104. as troughs in coverage at the
  7105. \begin_inset Flex Glossary Term
  7106. status open
  7107. \begin_layout Plain Layout
  7108. TSS
  7109. \end_layout
  7110. \end_inset
  7111. and asymmetric coverage upstream and downstream, so it is difficult in
  7112. this case to evaluate whether the 2.5
  7113. \begin_inset space ~
  7114. \end_inset
  7115. kb radius determined from TSS-to-peak distances is functionally significant.
  7116. However, the two patterns of coverage associated with elevated expression
  7117. levels both have interesting features within this radius.
  7118. \end_layout
  7119. \begin_layout Subsection
  7120. Convergence
  7121. \end_layout
  7122. \begin_layout Standard
  7123. \begin_inset Flex TODO Note (inline)
  7124. status open
  7125. \begin_layout Plain Layout
  7126. Look up some more references for these histone marks being involved in memory
  7127. differentiation.
  7128. (Ask Sarah)
  7129. \end_layout
  7130. \end_inset
  7131. \end_layout
  7132. \begin_layout Standard
  7133. We observed that all 3 histone marks and the gene expression data all exhibit
  7134. evidence of convergence in abundance between naïve and memory cells by
  7135. day 14 after activation (Figure
  7136. \begin_inset CommandInset ref
  7137. LatexCommand ref
  7138. reference "fig:PCoA-promoters"
  7139. plural "false"
  7140. caps "false"
  7141. noprefix "false"
  7142. \end_inset
  7143. , Table
  7144. \begin_inset CommandInset ref
  7145. LatexCommand ref
  7146. reference "tab:Number-signif-promoters"
  7147. plural "false"
  7148. caps "false"
  7149. noprefix "false"
  7150. \end_inset
  7151. ).
  7152. The
  7153. \begin_inset Flex Glossary Term
  7154. status open
  7155. \begin_layout Plain Layout
  7156. MOFA
  7157. \end_layout
  7158. \end_inset
  7159. \begin_inset Flex Glossary Term
  7160. status open
  7161. \begin_layout Plain Layout
  7162. LF
  7163. \end_layout
  7164. \end_inset
  7165. scatter plots (Figure
  7166. \begin_inset CommandInset ref
  7167. LatexCommand ref
  7168. reference "fig:mofa-lf-scatter"
  7169. plural "false"
  7170. caps "false"
  7171. noprefix "false"
  7172. \end_inset
  7173. ) show that this pattern of convergence is captured in
  7174. \begin_inset Flex Glossary Term
  7175. status open
  7176. \begin_layout Plain Layout
  7177. LF
  7178. \end_layout
  7179. \end_inset
  7180. 5.
  7181. Like all the
  7182. \begin_inset Flex Glossary Term (pl)
  7183. status open
  7184. \begin_layout Plain Layout
  7185. LF
  7186. \end_layout
  7187. \end_inset
  7188. in this plot, this factor explains a substantial portion of the variance
  7189. in all 4 data sets, indicating a coordinated pattern of variation shared
  7190. across all histone marks and gene expression.
  7191. This is consistent with the expectation that any naïve CD4
  7192. \begin_inset Formula $^{+}$
  7193. \end_inset
  7194. T-cells remaining at day 14 should have differentiated into memory cells
  7195. by that time, and should therefore have a genomic and epigenomic state
  7196. similar to memory cells.
  7197. This convergence is evidence that these histone marks all play an important
  7198. role in the naïve-to-memory differentiation process.
  7199. A histone mark that was not involved in naïve-to-memory differentiation
  7200. would not be expected to converge in this way after activation.
  7201. \end_layout
  7202. \begin_layout Standard
  7203. In H3K4me2, H3K4me3, and
  7204. \begin_inset Flex Glossary Term
  7205. status open
  7206. \begin_layout Plain Layout
  7207. RNA-seq
  7208. \end_layout
  7209. \end_inset
  7210. , this convergence appears to be in progress already by Day 5, shown by
  7211. the smaller distance between naïve and memory cells at day 5 along the
  7212. \begin_inset Formula $y$
  7213. \end_inset
  7214. -axes in Figures
  7215. \begin_inset CommandInset ref
  7216. LatexCommand ref
  7217. reference "fig:PCoA-H3K4me2-prom"
  7218. plural "false"
  7219. caps "false"
  7220. noprefix "false"
  7221. \end_inset
  7222. ,
  7223. \begin_inset CommandInset ref
  7224. LatexCommand ref
  7225. reference "fig:PCoA-H3K4me3-prom"
  7226. plural "false"
  7227. caps "false"
  7228. noprefix "false"
  7229. \end_inset
  7230. , and
  7231. \begin_inset CommandInset ref
  7232. LatexCommand ref
  7233. reference "fig:RNA-PCA-group"
  7234. plural "false"
  7235. caps "false"
  7236. noprefix "false"
  7237. \end_inset
  7238. .
  7239. This agrees with the model proposed by Sarah Lamere based on an prior analysis
  7240. of the same data, shown in Figure
  7241. \begin_inset CommandInset ref
  7242. LatexCommand ref
  7243. reference "fig:Lamere2016-Fig8"
  7244. plural "false"
  7245. caps "false"
  7246. noprefix "false"
  7247. \end_inset
  7248. , which shows the pattern of H3K4 methylation and expression for naïve cells
  7249. and memory cells converging at day 5.
  7250. This model was developed without the benefit of the
  7251. \begin_inset Flex Glossary Term
  7252. status open
  7253. \begin_layout Plain Layout
  7254. PCoA
  7255. \end_layout
  7256. \end_inset
  7257. plots in Figure
  7258. \begin_inset CommandInset ref
  7259. LatexCommand ref
  7260. reference "fig:PCoA-promoters"
  7261. plural "false"
  7262. caps "false"
  7263. noprefix "false"
  7264. \end_inset
  7265. , which have been corrected for confounding factors by ComBat and
  7266. \begin_inset Flex Glossary Term
  7267. status open
  7268. \begin_layout Plain Layout
  7269. SVA
  7270. \end_layout
  7271. \end_inset
  7272. .
  7273. This shows that proper batch correction assists in extracting meaningful
  7274. patterns in the data while eliminating systematic sources of irrelevant
  7275. variation in the data, allowing simple automated procedures like
  7276. \begin_inset Flex Glossary Term
  7277. status open
  7278. \begin_layout Plain Layout
  7279. PCoA
  7280. \end_layout
  7281. \end_inset
  7282. to reveal interesting behaviors in the data that were previously only detectabl
  7283. e by a detailed manual analysis.
  7284. While the ideal comparison to demonstrate this convergence would be naïve
  7285. cells at day 14 to memory cells at day 0, this is not feasible in this
  7286. experimental system, since neither naïve nor memory cells are able to fully
  7287. return to their pre-activation state, as shown by the lack of overlap between
  7288. days 0 and 14 for either naïve or memory cells in Figure
  7289. \begin_inset CommandInset ref
  7290. LatexCommand ref
  7291. reference "fig:PCoA-promoters"
  7292. plural "false"
  7293. caps "false"
  7294. noprefix "false"
  7295. \end_inset
  7296. .
  7297. \end_layout
  7298. \begin_layout Standard
  7299. \begin_inset Float figure
  7300. wide false
  7301. sideways false
  7302. status collapsed
  7303. \begin_layout Plain Layout
  7304. \align center
  7305. \begin_inset Graphics
  7306. filename graphics/CD4-csaw/LaMere2016_fig8.pdf
  7307. lyxscale 50
  7308. width 100col%
  7309. groupId colfullwidth
  7310. \end_inset
  7311. \end_layout
  7312. \begin_layout Plain Layout
  7313. \begin_inset Caption Standard
  7314. \begin_layout Plain Layout
  7315. \begin_inset Argument 1
  7316. status collapsed
  7317. \begin_layout Plain Layout
  7318. Lamere 2016 Figure 8 “Model for the role of H3K4 methylation during CD4
  7319. \begin_inset Formula $^{+}$
  7320. \end_inset
  7321. T-cell activation.
  7322. \begin_inset Quotes erd
  7323. \end_inset
  7324. \end_layout
  7325. \end_inset
  7326. \begin_inset CommandInset label
  7327. LatexCommand label
  7328. name "fig:Lamere2016-Fig8"
  7329. \end_inset
  7330. \series bold
  7331. Lamere 2016 Figure 8
  7332. \begin_inset CommandInset citation
  7333. LatexCommand cite
  7334. key "LaMere2016"
  7335. literal "false"
  7336. \end_inset
  7337. ,
  7338. \begin_inset Quotes eld
  7339. \end_inset
  7340. Model for the role of H3K4 methylation during CD4
  7341. \begin_inset Formula $\mathbf{^{+}}$
  7342. \end_inset
  7343. T-cell activation.
  7344. \begin_inset Quotes erd
  7345. \end_inset
  7346. \series default
  7347. (Reproduced with permission.)
  7348. \end_layout
  7349. \end_inset
  7350. \end_layout
  7351. \end_inset
  7352. \end_layout
  7353. \begin_layout Subsection
  7354. Positional
  7355. \end_layout
  7356. \begin_layout Standard
  7357. When looking at patterns in the relative coverage of each histone mark near
  7358. the
  7359. \begin_inset Flex Glossary Term
  7360. status open
  7361. \begin_layout Plain Layout
  7362. TSS
  7363. \end_layout
  7364. \end_inset
  7365. of each gene, several interesting patterns were apparent.
  7366. For H3K4me2 and H3K4me3, the pattern was straightforward: the consistent
  7367. pattern across all promoters was a single peak a few kb wide, with the
  7368. main axis of variation being the position of this peak relative to the
  7369. \begin_inset Flex Glossary Term
  7370. status open
  7371. \begin_layout Plain Layout
  7372. TSS
  7373. \end_layout
  7374. \end_inset
  7375. (Figures
  7376. \begin_inset CommandInset ref
  7377. LatexCommand ref
  7378. reference "fig:H3K4me2-neighborhood"
  7379. plural "false"
  7380. caps "false"
  7381. noprefix "false"
  7382. \end_inset
  7383. &
  7384. \begin_inset CommandInset ref
  7385. LatexCommand ref
  7386. reference "fig:H3K4me3-neighborhood"
  7387. plural "false"
  7388. caps "false"
  7389. noprefix "false"
  7390. \end_inset
  7391. ).
  7392. There were no obvious
  7393. \begin_inset Quotes eld
  7394. \end_inset
  7395. preferred
  7396. \begin_inset Quotes erd
  7397. \end_inset
  7398. positions, but rather a continuous distribution of relative positions ranging
  7399. all across the promoter region.
  7400. The association with gene expression was also straightforward: peaks closer
  7401. to the
  7402. \begin_inset Flex Glossary Term
  7403. status open
  7404. \begin_layout Plain Layout
  7405. TSS
  7406. \end_layout
  7407. \end_inset
  7408. were more strongly associated with elevated gene expression.
  7409. Coverage downstream of the
  7410. \begin_inset Flex Glossary Term
  7411. status open
  7412. \begin_layout Plain Layout
  7413. TSS
  7414. \end_layout
  7415. \end_inset
  7416. appears to be more strongly associated with elevated expression than coverage
  7417. at the same distance upstream, indicating that the
  7418. \begin_inset Quotes eld
  7419. \end_inset
  7420. effective promoter region
  7421. \begin_inset Quotes erd
  7422. \end_inset
  7423. for H3K4me2 and H3K4me3 may be centered downstream of the
  7424. \begin_inset Flex Glossary Term
  7425. status open
  7426. \begin_layout Plain Layout
  7427. TSS
  7428. \end_layout
  7429. \end_inset
  7430. .
  7431. \end_layout
  7432. \begin_layout Standard
  7433. The relative promoter coverage for H3K27me3 had a more complex pattern,
  7434. with two specific patterns of promoter coverage associated with elevated
  7435. expression: a sharp depletion of H3K27me3 around the
  7436. \begin_inset Flex Glossary Term
  7437. status open
  7438. \begin_layout Plain Layout
  7439. TSS
  7440. \end_layout
  7441. \end_inset
  7442. relative to the surrounding area, and a depletion of H3K27me3 downstream
  7443. of the
  7444. \begin_inset Flex Glossary Term
  7445. status open
  7446. \begin_layout Plain Layout
  7447. TSS
  7448. \end_layout
  7449. \end_inset
  7450. relative to upstream (Figure
  7451. \begin_inset CommandInset ref
  7452. LatexCommand ref
  7453. reference "fig:H3K27me3-neighborhood"
  7454. plural "false"
  7455. caps "false"
  7456. noprefix "false"
  7457. \end_inset
  7458. ).
  7459. A previous study found that H3K27me3 depletion within the gene body was
  7460. associated with elevated gene expression in 4 different cell types in mice
  7461. \begin_inset CommandInset citation
  7462. LatexCommand cite
  7463. key "Young2011"
  7464. literal "false"
  7465. \end_inset
  7466. .
  7467. This is consistent with the second pattern described here.
  7468. This study also reported that a spike in coverage at the
  7469. \begin_inset Flex Glossary Term
  7470. status open
  7471. \begin_layout Plain Layout
  7472. TSS
  7473. \end_layout
  7474. \end_inset
  7475. was associated with
  7476. \emph on
  7477. lower
  7478. \emph default
  7479. expression, which is indirectly consistent with the first pattern described
  7480. here, in the sense that it associates lower H3K27me3 levels near the
  7481. \begin_inset Flex Glossary Term
  7482. status open
  7483. \begin_layout Plain Layout
  7484. TSS
  7485. \end_layout
  7486. \end_inset
  7487. with higher expression.
  7488. \end_layout
  7489. \begin_layout Subsection
  7490. Workflow
  7491. \end_layout
  7492. \begin_layout Standard
  7493. The analyses described in this chapter were organized into a reproducible
  7494. workflow using the Snakemake workflow management system
  7495. \begin_inset CommandInset citation
  7496. LatexCommand cite
  7497. key "Koster2012"
  7498. literal "false"
  7499. \end_inset
  7500. .
  7501. As shown in Figure
  7502. \begin_inset CommandInset ref
  7503. LatexCommand ref
  7504. reference "fig:rulegraph"
  7505. plural "false"
  7506. caps "false"
  7507. noprefix "false"
  7508. \end_inset
  7509. , the workflow includes many steps with complex dependencies between them.
  7510. For example, the step that counts the number of
  7511. \begin_inset Flex Glossary Term
  7512. status open
  7513. \begin_layout Plain Layout
  7514. ChIP-seq
  7515. \end_layout
  7516. \end_inset
  7517. reads in 500
  7518. \begin_inset space ~
  7519. \end_inset
  7520. bp windows in each promoter (the starting point for Figures
  7521. \begin_inset CommandInset ref
  7522. LatexCommand ref
  7523. reference "fig:H3K4me2-neighborhood"
  7524. plural "false"
  7525. caps "false"
  7526. noprefix "false"
  7527. \end_inset
  7528. ,
  7529. \begin_inset CommandInset ref
  7530. LatexCommand ref
  7531. reference "fig:H3K4me3-neighborhood"
  7532. plural "false"
  7533. caps "false"
  7534. noprefix "false"
  7535. \end_inset
  7536. , and
  7537. \begin_inset CommandInset ref
  7538. LatexCommand ref
  7539. reference "fig:H3K27me3-neighborhood"
  7540. plural "false"
  7541. caps "false"
  7542. noprefix "false"
  7543. \end_inset
  7544. ), named
  7545. \begin_inset Flex Code
  7546. status open
  7547. \begin_layout Plain Layout
  7548. chipseq_count_tss_neighborhoods
  7549. \end_layout
  7550. \end_inset
  7551. , depends on the
  7552. \begin_inset Flex Glossary Term
  7553. status open
  7554. \begin_layout Plain Layout
  7555. RNA-seq
  7556. \end_layout
  7557. \end_inset
  7558. abundance estimates in order to select the most-used
  7559. \begin_inset Flex Glossary Term
  7560. status open
  7561. \begin_layout Plain Layout
  7562. TSS
  7563. \end_layout
  7564. \end_inset
  7565. for each gene, the aligned
  7566. \begin_inset Flex Glossary Term
  7567. status open
  7568. \begin_layout Plain Layout
  7569. ChIP-seq
  7570. \end_layout
  7571. \end_inset
  7572. reads, the index for those reads, and the blacklist of regions to be excluded
  7573. from
  7574. \begin_inset Flex Glossary Term
  7575. status open
  7576. \begin_layout Plain Layout
  7577. ChIP-seq
  7578. \end_layout
  7579. \end_inset
  7580. analysis.
  7581. Each step declares its inputs and outputs, and Snakemake uses these to
  7582. determine the dependencies between steps.
  7583. Each step is marked as depending on all the steps whose outputs match its
  7584. inputs, generating the workflow graph in Figure
  7585. \begin_inset CommandInset ref
  7586. LatexCommand ref
  7587. reference "fig:rulegraph"
  7588. plural "false"
  7589. caps "false"
  7590. noprefix "false"
  7591. \end_inset
  7592. , which Snakemake uses to determine order in which to execute each step
  7593. so that each step is executed only after all of the steps it depends on
  7594. have completed, thereby automating the entire workflow from start to finish.
  7595. \end_layout
  7596. \begin_layout Standard
  7597. \begin_inset ERT
  7598. status open
  7599. \begin_layout Plain Layout
  7600. \backslash
  7601. afterpage{
  7602. \end_layout
  7603. \begin_layout Plain Layout
  7604. \backslash
  7605. begin{landscape}
  7606. \end_layout
  7607. \end_inset
  7608. \end_layout
  7609. \begin_layout Standard
  7610. \begin_inset Float figure
  7611. wide false
  7612. sideways false
  7613. status collapsed
  7614. \begin_layout Plain Layout
  7615. \align center
  7616. \begin_inset Graphics
  7617. filename graphics/CD4-csaw/rulegraphs/rulegraph-all.pdf
  7618. lyxscale 50
  7619. width 100col%
  7620. height 95theight%
  7621. \end_inset
  7622. \end_layout
  7623. \begin_layout Plain Layout
  7624. \begin_inset Caption Standard
  7625. \begin_layout Plain Layout
  7626. \begin_inset Argument 1
  7627. status collapsed
  7628. \begin_layout Plain Layout
  7629. Dependency graph of steps in reproducible workflow.
  7630. \end_layout
  7631. \end_inset
  7632. \begin_inset CommandInset label
  7633. LatexCommand label
  7634. name "fig:rulegraph"
  7635. \end_inset
  7636. \series bold
  7637. Dependency graph of steps in reproducible workflow.
  7638. \series default
  7639. The analysis flows from left to right.
  7640. Arrows indicate which analysis steps depend on the output of other steps.
  7641. \end_layout
  7642. \end_inset
  7643. \end_layout
  7644. \end_inset
  7645. \end_layout
  7646. \begin_layout Standard
  7647. \begin_inset ERT
  7648. status open
  7649. \begin_layout Plain Layout
  7650. \backslash
  7651. end{landscape}
  7652. \end_layout
  7653. \begin_layout Plain Layout
  7654. }
  7655. \end_layout
  7656. \end_inset
  7657. \end_layout
  7658. \begin_layout Standard
  7659. In addition to simply making it easier to organize the steps in the analysis,
  7660. structuring the analysis as a workflow allowed for some analysis strategies
  7661. that would not have been practical otherwise.
  7662. For example, 5 different
  7663. \begin_inset Flex Glossary Term
  7664. status open
  7665. \begin_layout Plain Layout
  7666. RNA-seq
  7667. \end_layout
  7668. \end_inset
  7669. quantification methods were tested against two different reference transcriptom
  7670. e annotations for a total of 10 different quantifications of the same
  7671. \begin_inset Flex Glossary Term
  7672. status open
  7673. \begin_layout Plain Layout
  7674. RNA-seq
  7675. \end_layout
  7676. \end_inset
  7677. data.
  7678. These were then compared against each other in the exploratory data analysis
  7679. step, to determine that the results were not very sensitive to either the
  7680. choice of quantification method or the choice of annotation.
  7681. This was possible with a single script for the exploratory data analysis,
  7682. because Snakemake was able to automate running this script for every combinatio
  7683. n of method and reference.
  7684. In a similar manner, two different peak calling methods were tested against
  7685. each other, and in this case it was determined that
  7686. \begin_inset Flex Glossary Term
  7687. status open
  7688. \begin_layout Plain Layout
  7689. SICER
  7690. \end_layout
  7691. \end_inset
  7692. was unambiguously superior to
  7693. \begin_inset Flex Glossary Term
  7694. status open
  7695. \begin_layout Plain Layout
  7696. MACS
  7697. \end_layout
  7698. \end_inset
  7699. for all histone marks studied.
  7700. By enabling these types of comparisons, structuring the analysis as an
  7701. automated workflow allowed important analysis decisions to be made in a
  7702. data-driven way, by running every reasonable option through the downstream
  7703. steps, seeing the consequences of choosing each option, and deciding accordingl
  7704. y.
  7705. \end_layout
  7706. \begin_layout Subsection
  7707. Data quality issues limit conclusions
  7708. \end_layout
  7709. \begin_layout Standard
  7710. \begin_inset Flex TODO Note (inline)
  7711. status open
  7712. \begin_layout Plain Layout
  7713. Is this needed?
  7714. \end_layout
  7715. \end_inset
  7716. \end_layout
  7717. \begin_layout Section
  7718. Future Directions
  7719. \end_layout
  7720. \begin_layout Standard
  7721. The analysis of
  7722. \begin_inset Flex Glossary Term
  7723. status open
  7724. \begin_layout Plain Layout
  7725. RNA-seq
  7726. \end_layout
  7727. \end_inset
  7728. and
  7729. \begin_inset Flex Glossary Term
  7730. status open
  7731. \begin_layout Plain Layout
  7732. ChIP-seq
  7733. \end_layout
  7734. \end_inset
  7735. in CD4
  7736. \begin_inset Formula $^{+}$
  7737. \end_inset
  7738. T-cells in Chapter 2 is in many ways a preliminary study that suggests
  7739. a multitude of new avenues of investigation.
  7740. Here we consider a selection of such avenues.
  7741. \end_layout
  7742. \begin_layout Subsection
  7743. Negative results
  7744. \end_layout
  7745. \begin_layout Standard
  7746. Two additional analyses were conducted beyond those reported in the results.
  7747. First, we searched for evidence that the presence or absence of a
  7748. \begin_inset Flex Glossary Term
  7749. status open
  7750. \begin_layout Plain Layout
  7751. CpGi
  7752. \end_layout
  7753. \end_inset
  7754. in the promoter was correlated with increases or decreases in gene expression
  7755. or any histone mark in any of the tested contrasts.
  7756. Second, we searched for evidence that the relative
  7757. \begin_inset Flex Glossary Term
  7758. status open
  7759. \begin_layout Plain Layout
  7760. ChIP-seq
  7761. \end_layout
  7762. \end_inset
  7763. coverage profiles prior to activations could predict the change in expression
  7764. of a gene after activation.
  7765. Neither analysis turned up any clear positive results.
  7766. \end_layout
  7767. \begin_layout Subsection
  7768. Improve on the idea of an effective promoter radius
  7769. \end_layout
  7770. \begin_layout Standard
  7771. This study introduced the concept of an
  7772. \begin_inset Quotes eld
  7773. \end_inset
  7774. effective promoter radius
  7775. \begin_inset Quotes erd
  7776. \end_inset
  7777. specific to each histone mark based on distance from the
  7778. \begin_inset Flex Glossary Term
  7779. status open
  7780. \begin_layout Plain Layout
  7781. TSS
  7782. \end_layout
  7783. \end_inset
  7784. within which an excess of peaks was called for that mark.
  7785. This concept was then used to guide further analyses throughout the study.
  7786. However, while the effective promoter radius was useful in those analyses,
  7787. it is both limited in theory and shown in practice to be a possible oversimplif
  7788. ication.
  7789. First, the effective promoter radii used in this study were chosen based
  7790. on manual inspection of the TSS-to-peak distance distributions in Figure
  7791. \begin_inset CommandInset ref
  7792. LatexCommand ref
  7793. reference "fig:near-promoter-peak-enrich"
  7794. plural "false"
  7795. caps "false"
  7796. noprefix "false"
  7797. \end_inset
  7798. , selecting round numbers of analyst convenience (Table
  7799. \begin_inset CommandInset ref
  7800. LatexCommand ref
  7801. reference "tab:effective-promoter-radius"
  7802. plural "false"
  7803. caps "false"
  7804. noprefix "false"
  7805. \end_inset
  7806. ).
  7807. It would be better to define an algorithm that selects a more precise radius
  7808. based on the features of the graph.
  7809. One possible way to do this would be to randomly rearrange the called peaks
  7810. throughout the genome many (while preserving the distribution of peak widths)
  7811. and re-generate the same plot as in Figure
  7812. \begin_inset CommandInset ref
  7813. LatexCommand ref
  7814. reference "fig:near-promoter-peak-enrich"
  7815. plural "false"
  7816. caps "false"
  7817. noprefix "false"
  7818. \end_inset
  7819. .
  7820. This would yield a better
  7821. \begin_inset Quotes eld
  7822. \end_inset
  7823. background
  7824. \begin_inset Quotes erd
  7825. \end_inset
  7826. distribution that demonstrates the degree of near-TSS enrichment that would
  7827. be expected by random chance.
  7828. The effective promoter radius could be defined as the point where the true
  7829. distribution diverges from the randomized background distribution.
  7830. \end_layout
  7831. \begin_layout Standard
  7832. Furthermore, the above definition of effective promoter radius has the significa
  7833. nt limitation of being based on the peak calling method.
  7834. It is thus very sensitive to the choice of peak caller and significance
  7835. threshold for calling peaks, as well as the degree of saturation in the
  7836. sequencing.
  7837. Calling peaks from
  7838. \begin_inset Flex Glossary Term
  7839. status open
  7840. \begin_layout Plain Layout
  7841. ChIP-seq
  7842. \end_layout
  7843. \end_inset
  7844. samples with insufficient coverage depth, with the wrong peak caller, or
  7845. with a different significance threshold could give a drastically different
  7846. number of called peaks, and hence a drastically different distribution
  7847. of peak-to-TSS distances.
  7848. To address this, it is desirable to develop a better method of determining
  7849. the effective promoter radius that relies only on the distribution of read
  7850. coverage around the
  7851. \begin_inset Flex Glossary Term
  7852. status open
  7853. \begin_layout Plain Layout
  7854. TSS
  7855. \end_layout
  7856. \end_inset
  7857. , independent of the peak calling.
  7858. Furthermore, as demonstrated by the upstream-downstream asymmetries observed
  7859. in Figures
  7860. \begin_inset CommandInset ref
  7861. LatexCommand ref
  7862. reference "fig:H3K4me2-neighborhood"
  7863. plural "false"
  7864. caps "false"
  7865. noprefix "false"
  7866. \end_inset
  7867. ,
  7868. \begin_inset CommandInset ref
  7869. LatexCommand ref
  7870. reference "fig:H3K4me3-neighborhood"
  7871. plural "false"
  7872. caps "false"
  7873. noprefix "false"
  7874. \end_inset
  7875. , and
  7876. \begin_inset CommandInset ref
  7877. LatexCommand ref
  7878. reference "fig:H3K27me3-neighborhood"
  7879. plural "false"
  7880. caps "false"
  7881. noprefix "false"
  7882. \end_inset
  7883. , this definition should determine a different radius for the upstream and
  7884. downstream directions.
  7885. At this point, it may be better to rename this concept
  7886. \begin_inset Quotes eld
  7887. \end_inset
  7888. effective promoter extent
  7889. \begin_inset Quotes erd
  7890. \end_inset
  7891. and avoid the word
  7892. \begin_inset Quotes eld
  7893. \end_inset
  7894. radius
  7895. \begin_inset Quotes erd
  7896. \end_inset
  7897. , since a radius implies a symmetry about the
  7898. \begin_inset Flex Glossary Term
  7899. status open
  7900. \begin_layout Plain Layout
  7901. TSS
  7902. \end_layout
  7903. \end_inset
  7904. that is not supported by the data.
  7905. \end_layout
  7906. \begin_layout Standard
  7907. Beyond improving the definition of effective promoter extent, functional
  7908. validation is necessary to show that this measure of near-TSS enrichment
  7909. has biological meaning.
  7910. Figures
  7911. \begin_inset CommandInset ref
  7912. LatexCommand ref
  7913. reference "fig:H3K4me2-neighborhood"
  7914. plural "false"
  7915. caps "false"
  7916. noprefix "false"
  7917. \end_inset
  7918. and
  7919. \begin_inset CommandInset ref
  7920. LatexCommand ref
  7921. reference "fig:H3K4me3-neighborhood"
  7922. plural "false"
  7923. caps "false"
  7924. noprefix "false"
  7925. \end_inset
  7926. already provide a very limited functional validation of the chosen promoter
  7927. extents for H3K4me2 and H3K4me3 by showing that spikes in coverage within
  7928. this region are most strongly correlated with elevated gene expression.
  7929. However, there are other ways to show functional relevance of the promoter
  7930. extent.
  7931. For example, correlations could be computed between read counts in peaks
  7932. nearby gene promoters and the expression level of those genes, and these
  7933. correlations could be plotted against the distance of the peak upstream
  7934. or downstream of the gene's
  7935. \begin_inset Flex Glossary Term
  7936. status open
  7937. \begin_layout Plain Layout
  7938. TSS
  7939. \end_layout
  7940. \end_inset
  7941. .
  7942. If the promoter extent truly defines a
  7943. \begin_inset Quotes eld
  7944. \end_inset
  7945. sphere of influence
  7946. \begin_inset Quotes erd
  7947. \end_inset
  7948. within which a histone mark is involved with the regulation of a gene,
  7949. then the correlations for peaks within this extent should be significantly
  7950. higher than those further upstream or downstream.
  7951. Peaks within these extents may also be more likely to show differential
  7952. modification than those outside genic regions of the genome.
  7953. \end_layout
  7954. \begin_layout Subsection
  7955. Design experiments to focus on post-activation convergence of naïve & memory
  7956. cells
  7957. \end_layout
  7958. \begin_layout Standard
  7959. In this study, a convergence between naïve and memory cells was observed
  7960. in both the pattern of gene expression and in epigenetic state of the 3
  7961. histone marks studied, consistent with the hypothesis that any naïve cells
  7962. remaining 14 days after activation have differentiated into memory cells,
  7963. and that both gene expression and these histone marks are involved in this
  7964. differentiation.
  7965. However, the current study was not designed with this specific hypothesis
  7966. in mind, and it therefore has some deficiencies with regard to testing
  7967. it.
  7968. The memory CD4
  7969. \begin_inset Formula $^{+}$
  7970. \end_inset
  7971. samples at day 14 do not resemble the memory samples at day 0, indicating
  7972. that in the specific model of activation used for this experiment, the
  7973. cells are not guaranteed to return to their original pre-activation state,
  7974. or perhaps this process takes substantially longer than 14 days.
  7975. This is a challenge for the convergence hypothesis because the ideal comparison
  7976. to prove that naïve cells are converging to a resting memory state would
  7977. be to compare the final naïve time point to the Day 0 memory samples, but
  7978. this comparison is only meaningful if memory cells generally return to
  7979. the same
  7980. \begin_inset Quotes eld
  7981. \end_inset
  7982. resting
  7983. \begin_inset Quotes erd
  7984. \end_inset
  7985. state that they started at.
  7986. \end_layout
  7987. \begin_layout Standard
  7988. To better study the convergence hypothesis, a new experiment should be designed
  7989. using a model system for T-cell activation that is known to allow cells
  7990. to return as closely as possible to their pre-activation state.
  7991. Alternatively, if it is not possible to find or design such a model system,
  7992. the same cell cultures could be activated serially multiple times, and
  7993. sequenced after each activation cycle right before the next activation.
  7994. It is likely that several activations in the same model system will settle
  7995. into a cyclical pattern, converging to a consistent
  7996. \begin_inset Quotes eld
  7997. \end_inset
  7998. resting
  7999. \begin_inset Quotes erd
  8000. \end_inset
  8001. state after each activation, even if this state is different from the initial
  8002. resting state at Day 0.
  8003. If so, it will be possible to compare the final states of both naïve and
  8004. memory cells to show that they converge despite different initial conditions.
  8005. \end_layout
  8006. \begin_layout Standard
  8007. In addition, if naïve-to-memory convergence is a general pattern, it should
  8008. also be detectable in other epigenetic marks, including other histone marks
  8009. and DNA methylation.
  8010. An experiment should be designed studying a large number of epigenetic
  8011. marks known or suspected to be involved in regulation of gene expression,
  8012. assaying all of these at the same pre- and post-activation time points.
  8013. Multi-dataset factor analysis methods like
  8014. \begin_inset Flex Glossary Term
  8015. status open
  8016. \begin_layout Plain Layout
  8017. MOFA
  8018. \end_layout
  8019. \end_inset
  8020. can then be used to identify coordinated patterns of regulation shared
  8021. across many epigenetic marks.
  8022. If possible, some
  8023. \begin_inset Quotes eld
  8024. \end_inset
  8025. negative control
  8026. \begin_inset Quotes erd
  8027. \end_inset
  8028. marks should be included that are known
  8029. \emph on
  8030. not
  8031. \emph default
  8032. to be involved in T-cell activation or memory formation.
  8033. Of course, CD4
  8034. \begin_inset Formula $^{+}$
  8035. \end_inset
  8036. T-cells are not the only adaptive immune cells with memory.
  8037. A similar study could be designed for CD8
  8038. \begin_inset Formula $^{+}$
  8039. \end_inset
  8040. T-cells, B-cells, and even specific subsets of CD4
  8041. \begin_inset Formula $^{+}$
  8042. \end_inset
  8043. T-cells, such as ???.
  8044. \end_layout
  8045. \begin_layout Standard
  8046. \begin_inset Flex TODO Note (inline)
  8047. status open
  8048. \begin_layout Plain Layout
  8049. Suggest some T-cell subsets
  8050. \end_layout
  8051. \end_inset
  8052. \end_layout
  8053. \begin_layout Subsection
  8054. Follow up on hints of interesting patterns in promoter relative coverage
  8055. profiles
  8056. \end_layout
  8057. \begin_layout Standard
  8058. \begin_inset Flex TODO Note (inline)
  8059. status open
  8060. \begin_layout Plain Layout
  8061. I think I might need to write up the negative results for the Promoter CpG
  8062. and defined pattern analysis before writing this section.
  8063. \end_layout
  8064. \end_inset
  8065. \end_layout
  8066. \begin_layout Itemize
  8067. Also find better normalizations: maybe borrow from MACS/SICER background
  8068. correction methods?
  8069. \end_layout
  8070. \begin_layout Itemize
  8071. For H3K4, define polar coordinates based on PC1 & 2: R = peak size, Theta
  8072. = peak position.
  8073. Then correlate with expression.
  8074. \end_layout
  8075. \begin_layout Standard
  8076. A better representation might be something like a polar coordinate system
  8077. with the origin at the center of Cluster 5, where the radius represents
  8078. the peak height above the background and the angle represents the peak's
  8079. position upstream or downstream of the
  8080. \begin_inset Flex Glossary Term
  8081. status open
  8082. \begin_layout Plain Layout
  8083. TSS
  8084. \end_layout
  8085. \end_inset
  8086. .
  8087. \end_layout
  8088. \begin_layout Itemize
  8089. Current analysis only at Day 0.
  8090. Need to study across time points.
  8091. \end_layout
  8092. \begin_layout Itemize
  8093. Integrating data across so many dimensions is a significant analysis challenge
  8094. \end_layout
  8095. \begin_layout Subsection
  8096. Investigate causes of high correlation between mutually exclusive histone
  8097. marks
  8098. \end_layout
  8099. \begin_layout Standard
  8100. The high correlation between coverage depth observed between H3K4me2 and
  8101. H3K4me3 is both expected and unexpected.
  8102. Since both marks are associated with elevated gene transcription, a positive
  8103. correlation between them is not surprising.
  8104. However, these two marks represent different post-translational modifications
  8105. of the
  8106. \emph on
  8107. same
  8108. \emph default
  8109. lysine residue on the histone H3 polypeptide, which means that they cannot
  8110. both be present on the same H3 subunit.
  8111. Thus, the high correlation between them has several potential explanations.
  8112. One possible reason is cell population heterogeneity: perhaps some genomic
  8113. loci are frequently marked with H3K4me2 in some cells, while in other cells
  8114. the same loci are marked with H3K4me3.
  8115. Another possibility is allele-specific modifications: the loci are marked
  8116. in each diploid cell with H3K4me2 on one allele and H3K4me3 on the other
  8117. allele.
  8118. Lastly, since each histone octamer contains 2 H3 subunits, it is possible
  8119. that having one H3K4me2 mark and one H3K4me3 mark on a given histone octamer
  8120. represents a distinct epigenetic state with a different function than either
  8121. double H3K4me2 or double H3K4me3.
  8122. \end_layout
  8123. \begin_layout Standard
  8124. These three hypotheses could be disentangled by single-cell
  8125. \begin_inset Flex Glossary Term
  8126. status open
  8127. \begin_layout Plain Layout
  8128. ChIP-seq
  8129. \end_layout
  8130. \end_inset
  8131. .
  8132. If the correlation between these two histone marks persists even within
  8133. the reads for each individual cell, then cell population heterogeneity
  8134. cannot explain the correlation.
  8135. Allele-specific modification can be tested for by looking at the correlation
  8136. between read coverage of the two histone marks at heterozygous loci.
  8137. If the correlation between read counts for opposite loci is low, then this
  8138. is consistent with allele-specific modification.
  8139. Finally if the modifications do not separate by either cell or allele,
  8140. the co-location of these two marks is most likely occurring at the level
  8141. of individual histones, with the heterogeneously modified histone representing
  8142. a distinct state.
  8143. \end_layout
  8144. \begin_layout Standard
  8145. However, another experiment would be required to show direct evidence of
  8146. such a heterogeneously modified state.
  8147. Specifically a
  8148. \begin_inset Quotes eld
  8149. \end_inset
  8150. double ChIP
  8151. \begin_inset Quotes erd
  8152. \end_inset
  8153. experiment would need to be performed, where the input DNA is first subjected
  8154. to an immunoprecipitation pulldown from the anti-H3K4me2 antibody, and
  8155. then the enriched material is collected, with proteins still bound, and
  8156. immunoprecipitated
  8157. \emph on
  8158. again
  8159. \emph default
  8160. using the anti-H3K4me3 antibody.
  8161. If this yields significant numbers of non-artifactual reads in the same
  8162. regions as the individual pulldowns of the two marks, this is strong evidence
  8163. that the two marks are occurring on opposite H3 subunits of the same histones.
  8164. \end_layout
  8165. \begin_layout Standard
  8166. \begin_inset Flex TODO Note (inline)
  8167. status open
  8168. \begin_layout Plain Layout
  8169. Try to see if double ChIP-seq is actually feasible, and if not, come up
  8170. with some other idea for directly detecting the mixed mod state.
  8171. Oh! Actually ChIP-seq isn't required, only double ChIP followed by quantificati
  8172. on.
  8173. That's one possible angle.
  8174. \end_layout
  8175. \end_inset
  8176. \end_layout
  8177. \begin_layout Chapter
  8178. Improving array-based diagnostics for transplant rejection by optimizing
  8179. data preprocessing
  8180. \end_layout
  8181. \begin_layout Standard
  8182. \size large
  8183. Ryan C.
  8184. Thompson, Sunil M.
  8185. Kurian, Thomas Whisnant, Padmaja Natarajan, Daniel R.
  8186. Salomon
  8187. \end_layout
  8188. \begin_layout Standard
  8189. \begin_inset ERT
  8190. status collapsed
  8191. \begin_layout Plain Layout
  8192. \backslash
  8193. glsresetall
  8194. \end_layout
  8195. \end_inset
  8196. \begin_inset Note Note
  8197. status collapsed
  8198. \begin_layout Plain Layout
  8199. Reintroduce all abbreviations
  8200. \end_layout
  8201. \end_inset
  8202. \end_layout
  8203. \begin_layout Section
  8204. Approach
  8205. \end_layout
  8206. \begin_layout Subsection
  8207. Proper pre-processing is essential for array data
  8208. \end_layout
  8209. \begin_layout Standard
  8210. Microarrays, bead arrays, and similar assays produce raw data in the form
  8211. of fluorescence intensity measurements, with each intensity measurement
  8212. proportional to the abundance of some fluorescently labelled target DNA
  8213. or RNA sequence that base pairs to a specific probe sequence.
  8214. However, these measurements for each probe are also affected my many technical
  8215. confounding factors, such as the concentration of target material, strength
  8216. of off-target binding, the sensitivity of the imaging sensor, and visual
  8217. artifacts in the image.
  8218. Some array designs also use multiple probe sequences for each target.
  8219. Hence, extensive pre-processing of array data is necessary to normalize
  8220. out the effects of these technical factors and summarize the information
  8221. from multiple probes to arrive at a single usable estimate of abundance
  8222. or other relevant quantity, such as a ratio of two abundances, for each
  8223. target
  8224. \begin_inset CommandInset citation
  8225. LatexCommand cite
  8226. key "Gentleman2005"
  8227. literal "false"
  8228. \end_inset
  8229. .
  8230. \end_layout
  8231. \begin_layout Standard
  8232. The choice of pre-processing algorithms used in the analysis of an array
  8233. data set can have a large effect on the results of that analysis.
  8234. However, despite their importance, these steps are often neglected or rushed
  8235. in order to get to the more scientifically interesting analysis steps involving
  8236. the actual biology of the system under study.
  8237. Hence, it is often possible to achieve substantial gains in statistical
  8238. power, model goodness-of-fit, or other relevant performance measures, by
  8239. checking the assumptions made by each preprocessing step and choosing specific
  8240. normalization methods tailored to the specific goals of the current analysis.
  8241. \end_layout
  8242. \begin_layout Subsection
  8243. Clinical diagnostic applications for microarrays require single-channel
  8244. normalization
  8245. \end_layout
  8246. \begin_layout Standard
  8247. As the cost of performing microarray assays falls, there is increasing interest
  8248. in using genomic assays for diagnostic purposes, such as distinguishing
  8249. \begin_inset ERT
  8250. status collapsed
  8251. \begin_layout Plain Layout
  8252. \backslash
  8253. glsdisp*{TX}{healthy transplants (TX)}
  8254. \end_layout
  8255. \end_inset
  8256. from transplants undergoing
  8257. \begin_inset Flex Glossary Term
  8258. status open
  8259. \begin_layout Plain Layout
  8260. AR
  8261. \end_layout
  8262. \end_inset
  8263. or
  8264. \begin_inset Flex Glossary Term
  8265. status open
  8266. \begin_layout Plain Layout
  8267. ADNR
  8268. \end_layout
  8269. \end_inset
  8270. .
  8271. However, the the standard normalization algorithm used for microarray data,
  8272. \begin_inset Flex Glossary Term
  8273. status open
  8274. \begin_layout Plain Layout
  8275. RMA
  8276. \end_layout
  8277. \end_inset
  8278. \begin_inset CommandInset citation
  8279. LatexCommand cite
  8280. key "Irizarry2003a"
  8281. literal "false"
  8282. \end_inset
  8283. , is not applicable in a clinical setting.
  8284. Two of the steps in
  8285. \begin_inset Flex Glossary Term
  8286. status open
  8287. \begin_layout Plain Layout
  8288. RMA
  8289. \end_layout
  8290. \end_inset
  8291. , quantile normalization and probe summarization by median polish, depend
  8292. on every array in the data set being normalized.
  8293. This means that adding or removing any arrays from a data set changes the
  8294. normalized values for all arrays, and data sets that have been normalized
  8295. separately cannot be compared to each other.
  8296. Hence, when using
  8297. \begin_inset Flex Glossary Term
  8298. status open
  8299. \begin_layout Plain Layout
  8300. RMA
  8301. \end_layout
  8302. \end_inset
  8303. , any arrays to be analyzed together must also be normalized together, and
  8304. the set of arrays included in the data set must be held constant throughout
  8305. an analysis.
  8306. \end_layout
  8307. \begin_layout Standard
  8308. These limitations present serious impediments to the use of arrays as a
  8309. diagnostic tool.
  8310. When training a classifier, the samples to be classified must not be involved
  8311. in any step of the training process, lest their inclusion bias the training
  8312. process.
  8313. Once a classifier is deployed in a clinical setting, the samples to be
  8314. classified will not even
  8315. \emph on
  8316. exist
  8317. \emph default
  8318. at the time of training, so including them would be impossible even if
  8319. it were statistically justifiable.
  8320. Therefore, any machine learning application for microarrays demands that
  8321. the normalized expression values computed for an array must depend only
  8322. on information contained within that array.
  8323. This would ensure that each array's normalization is independent of every
  8324. other array, and that arrays normalized separately can still be compared
  8325. to each other without bias.
  8326. Such a normalization is commonly referred to as
  8327. \begin_inset Quotes eld
  8328. \end_inset
  8329. single-channel normalization
  8330. \begin_inset Quotes erd
  8331. \end_inset
  8332. .
  8333. \end_layout
  8334. \begin_layout Standard
  8335. \begin_inset Flex Glossary Term (Capital)
  8336. status open
  8337. \begin_layout Plain Layout
  8338. fRMA
  8339. \end_layout
  8340. \end_inset
  8341. addresses these concerns by replacing the quantile normalization and median
  8342. polish with alternatives that do not introduce inter-array dependence,
  8343. allowing each array to be normalized independently of all others
  8344. \begin_inset CommandInset citation
  8345. LatexCommand cite
  8346. key "McCall2010"
  8347. literal "false"
  8348. \end_inset
  8349. .
  8350. Quantile normalization is performed against a pre-generated set of quantiles
  8351. learned from a collection of 850 publicly available arrays sampled from
  8352. a wide variety of tissues in
  8353. \begin_inset ERT
  8354. status collapsed
  8355. \begin_layout Plain Layout
  8356. \backslash
  8357. glsdisp*{GEO}{the Gene Expression Omnibus (GEO)}
  8358. \end_layout
  8359. \end_inset
  8360. .
  8361. Each array's probe intensity distribution is normalized against these pre-gener
  8362. ated quantiles.
  8363. The median polish step is replaced with a robust weighted average of probe
  8364. intensities, using inverse variance weights learned from the same public
  8365. \begin_inset Flex Glossary Term
  8366. status open
  8367. \begin_layout Plain Layout
  8368. GEO
  8369. \end_layout
  8370. \end_inset
  8371. data.
  8372. The result is a normalization that satisfies the requirements mentioned
  8373. above: each array is normalized independently of all others, and any two
  8374. normalized arrays can be compared directly to each other.
  8375. \end_layout
  8376. \begin_layout Standard
  8377. One important limitation of
  8378. \begin_inset Flex Glossary Term
  8379. status open
  8380. \begin_layout Plain Layout
  8381. fRMA
  8382. \end_layout
  8383. \end_inset
  8384. is that it requires a separate reference data set from which to learn the
  8385. parameters (reference quantiles and probe weights) that will be used to
  8386. normalize each array.
  8387. These parameters are specific to a given array platform, and pre-generated
  8388. parameters are only provided for the most common platforms, such as Affymetrix
  8389. hgu133plus2.
  8390. For a less common platform, such as hthgu133pluspm, is is necessary to
  8391. learn custom parameters from in-house data before
  8392. \begin_inset Flex Glossary Term
  8393. status open
  8394. \begin_layout Plain Layout
  8395. fRMA
  8396. \end_layout
  8397. \end_inset
  8398. can be used to normalize samples on that platform
  8399. \begin_inset CommandInset citation
  8400. LatexCommand cite
  8401. key "McCall2011"
  8402. literal "false"
  8403. \end_inset
  8404. .
  8405. \end_layout
  8406. \begin_layout Standard
  8407. One other option is the aptly-named
  8408. \begin_inset ERT
  8409. status collapsed
  8410. \begin_layout Plain Layout
  8411. \backslash
  8412. glsdisp*{SCAN}{Single Channel Array Normalization (SCAN)}
  8413. \end_layout
  8414. \end_inset
  8415. , which adapts a normalization method originally designed for tiling arrays
  8416. \begin_inset CommandInset citation
  8417. LatexCommand cite
  8418. key "Piccolo2012"
  8419. literal "false"
  8420. \end_inset
  8421. .
  8422. \begin_inset Flex Glossary Term
  8423. status open
  8424. \begin_layout Plain Layout
  8425. SCAN
  8426. \end_layout
  8427. \end_inset
  8428. is truly single-channel in that it does not require a set of normalization
  8429. parameters estimated from an external set of reference samples like
  8430. \begin_inset Flex Glossary Term
  8431. status open
  8432. \begin_layout Plain Layout
  8433. fRMA
  8434. \end_layout
  8435. \end_inset
  8436. does.
  8437. \end_layout
  8438. \begin_layout Subsection
  8439. Heteroskedasticity must be accounted for in methylation array data
  8440. \end_layout
  8441. \begin_layout Standard
  8442. DNA methylation arrays are a relatively new kind of assay that uses microarrays
  8443. to measure the degree of methylation on cytosines in specific regions arrayed
  8444. across the genome.
  8445. First, bisulfite treatment converts all unmethylated cytosines to uracil
  8446. (which are read as thymine during amplification and sequencing) while leaving
  8447. methylated cytosines unaffected.
  8448. Then, each target region is interrogated with two probes: one binds to
  8449. the original genomic sequence and interrogates the level of methylated
  8450. DNA, and the other binds to the same sequence with all cytosines replaced
  8451. by thymidines and interrogates the level of unmethylated DNA.
  8452. \end_layout
  8453. \begin_layout Standard
  8454. After normalization, these two probe intensities are summarized in one of
  8455. two ways, each with advantages and disadvantages.
  8456. β
  8457. \series bold
  8458. \series default
  8459. values, interpreted as fraction of DNA copies methylated, range from 0 to
  8460. 1.
  8461. β
  8462. \series bold
  8463. \series default
  8464. values are conceptually easy to interpret, but the constrained range makes
  8465. them unsuitable for linear modeling, and their error distributions are
  8466. highly non-normal, which also frustrates linear modeling.
  8467. \begin_inset ERT
  8468. status collapsed
  8469. \begin_layout Plain Layout
  8470. \backslash
  8471. glsdisp*{M-value}{M-values}
  8472. \end_layout
  8473. \end_inset
  8474. , interpreted as the log ratios of methylated to unmethylated copies for
  8475. each probe region, are computed by mapping the beta values from
  8476. \begin_inset Formula $[0,1]$
  8477. \end_inset
  8478. onto
  8479. \begin_inset Formula $(-\infty,+\infty)$
  8480. \end_inset
  8481. using a sigmoid curve (Figure
  8482. \begin_inset CommandInset ref
  8483. LatexCommand ref
  8484. reference "fig:Sigmoid-beta-m-mapping"
  8485. plural "false"
  8486. caps "false"
  8487. noprefix "false"
  8488. \end_inset
  8489. ).
  8490. This transformation results in values with better statistical properties:
  8491. the unconstrained range is suitable for linear modeling, and the error
  8492. distributions are more normal.
  8493. Hence, most linear modeling and other statistical testing on methylation
  8494. arrays is performed using
  8495. \begin_inset Flex Glossary Term (pl)
  8496. status open
  8497. \begin_layout Plain Layout
  8498. M-value
  8499. \end_layout
  8500. \end_inset
  8501. .
  8502. \end_layout
  8503. \begin_layout Standard
  8504. \begin_inset Float figure
  8505. wide false
  8506. sideways false
  8507. status open
  8508. \begin_layout Plain Layout
  8509. \align center
  8510. \begin_inset Graphics
  8511. filename graphics/methylvoom/sigmoid.pdf
  8512. lyxscale 50
  8513. width 60col%
  8514. groupId colwidth
  8515. \end_inset
  8516. \end_layout
  8517. \begin_layout Plain Layout
  8518. \begin_inset Caption Standard
  8519. \begin_layout Plain Layout
  8520. \begin_inset Argument 1
  8521. status collapsed
  8522. \begin_layout Plain Layout
  8523. Sigmoid shape of the mapping between β and M values.
  8524. \end_layout
  8525. \end_inset
  8526. \begin_inset CommandInset label
  8527. LatexCommand label
  8528. name "fig:Sigmoid-beta-m-mapping"
  8529. \end_inset
  8530. \series bold
  8531. Sigmoid shape of the mapping between β and M values.
  8532. \series default
  8533. This mapping is monotonic and non-linear, but it is approximately linear
  8534. in the neighborhood of
  8535. \begin_inset Formula $(\beta=0.5,M=0)$
  8536. \end_inset
  8537. .
  8538. \end_layout
  8539. \end_inset
  8540. \end_layout
  8541. \end_inset
  8542. \end_layout
  8543. \begin_layout Standard
  8544. However, the steep slope of the sigmoid transformation near 0 and 1 tends
  8545. to over-exaggerate small differences in β values near those extremes, which
  8546. in turn amplifies the error in those values, leading to a U-shaped trend
  8547. in the mean-variance curve: extreme values have higher variances than values
  8548. near the middle.
  8549. This mean-variance dependency must be accounted for when fitting the linear
  8550. model for differential methylation, or else the variance will be systematically
  8551. overestimated for probes with moderate
  8552. \begin_inset Flex Glossary Term (pl)
  8553. status open
  8554. \begin_layout Plain Layout
  8555. M-value
  8556. \end_layout
  8557. \end_inset
  8558. and underestimated for probes with extreme
  8559. \begin_inset Flex Glossary Term (pl)
  8560. status open
  8561. \begin_layout Plain Layout
  8562. M-value
  8563. \end_layout
  8564. \end_inset
  8565. .
  8566. This is particularly undesirable for methylation data because the intermediate
  8567. \begin_inset Flex Glossary Term (pl)
  8568. status open
  8569. \begin_layout Plain Layout
  8570. M-value
  8571. \end_layout
  8572. \end_inset
  8573. are the ones of most interest, since they are more likely to represent
  8574. areas of varying methylation, whereas extreme
  8575. \begin_inset Flex Glossary Term (pl)
  8576. status open
  8577. \begin_layout Plain Layout
  8578. M-value
  8579. \end_layout
  8580. \end_inset
  8581. typically represent complete methylation or complete lack of methylation.
  8582. \end_layout
  8583. \begin_layout Standard
  8584. \begin_inset Flex Glossary Term (Capital)
  8585. status open
  8586. \begin_layout Plain Layout
  8587. RNA-seq
  8588. \end_layout
  8589. \end_inset
  8590. read count data are also known to show heteroskedasticity, and the voom
  8591. method was introduced for modeling this heteroskedasticity by estimating
  8592. the mean-variance trend in the data and using this trend to assign precision
  8593. weights to each observation
  8594. \begin_inset CommandInset citation
  8595. LatexCommand cite
  8596. key "Law2013"
  8597. literal "false"
  8598. \end_inset
  8599. .
  8600. While methylation array data are not derived from counts and have a very
  8601. different mean-variance relationship from that of typical
  8602. \begin_inset Flex Glossary Term
  8603. status open
  8604. \begin_layout Plain Layout
  8605. RNA-seq
  8606. \end_layout
  8607. \end_inset
  8608. data, the voom method makes no specific assumptions on the shape of the
  8609. mean-variance relationship – it only assumes that the relationship can
  8610. be modeled as a smooth curve.
  8611. Hence, the method is sufficiently general to model the mean-variance relationsh
  8612. ip in methylation array data.
  8613. However, the standard implementation of voom assumes that the input is
  8614. given in raw read counts, and it must be adapted to run on methylation
  8615. \begin_inset Flex Glossary Term (pl)
  8616. status open
  8617. \begin_layout Plain Layout
  8618. M-value
  8619. \end_layout
  8620. \end_inset
  8621. .
  8622. \end_layout
  8623. \begin_layout Section
  8624. Methods
  8625. \end_layout
  8626. \begin_layout Subsection
  8627. Evaluation of classifier performance with different normalization methods
  8628. \end_layout
  8629. \begin_layout Standard
  8630. For testing different expression microarray normalizations, a data set of
  8631. 157 hgu133plus2 arrays was used, consisting of blood samples from kidney
  8632. transplant patients whose grafts had been graded as
  8633. \begin_inset Flex Glossary Term
  8634. status open
  8635. \begin_layout Plain Layout
  8636. TX
  8637. \end_layout
  8638. \end_inset
  8639. ,
  8640. \begin_inset Flex Glossary Term
  8641. status open
  8642. \begin_layout Plain Layout
  8643. AR
  8644. \end_layout
  8645. \end_inset
  8646. , or
  8647. \begin_inset Flex Glossary Term
  8648. status open
  8649. \begin_layout Plain Layout
  8650. ADNR
  8651. \end_layout
  8652. \end_inset
  8653. via biopsy and histology (46 TX, 69 AR, 42 ADNR)
  8654. \begin_inset CommandInset citation
  8655. LatexCommand cite
  8656. key "Kurian2014"
  8657. literal "true"
  8658. \end_inset
  8659. .
  8660. Additionally, an external validation set of 75 samples was gathered from
  8661. public
  8662. \begin_inset Flex Glossary Term
  8663. status open
  8664. \begin_layout Plain Layout
  8665. GEO
  8666. \end_layout
  8667. \end_inset
  8668. data (37 TX, 38 AR, no ADNR).
  8669. \end_layout
  8670. \begin_layout Standard
  8671. \begin_inset Flex TODO Note (inline)
  8672. status open
  8673. \begin_layout Plain Layout
  8674. Find appropriate GEO identifiers if possible.
  8675. Kurian 2014 says GSE15296, but this seems to be different data.
  8676. I also need to look up the GEO accession for the external validation set.
  8677. \end_layout
  8678. \end_inset
  8679. \end_layout
  8680. \begin_layout Standard
  8681. To evaluate the effect of each normalization on classifier performance,
  8682. the same classifier training and validation procedure was used after each
  8683. normalization method.
  8684. The
  8685. \begin_inset Flex Glossary Term
  8686. status open
  8687. \begin_layout Plain Layout
  8688. PAM
  8689. \end_layout
  8690. \end_inset
  8691. algorithm was used to train a nearest shrunken centroid classifier on the
  8692. training set and select the appropriate threshold for centroid shrinking
  8693. \begin_inset CommandInset citation
  8694. LatexCommand cite
  8695. key "Tibshirani2002"
  8696. literal "false"
  8697. \end_inset
  8698. .
  8699. Then the trained classifier was used to predict the class probabilities
  8700. of each validation sample.
  8701. From these class probabilities,
  8702. \begin_inset Flex Glossary Term
  8703. status open
  8704. \begin_layout Plain Layout
  8705. ROC
  8706. \end_layout
  8707. \end_inset
  8708. curves and
  8709. \begin_inset Flex Glossary Term
  8710. status open
  8711. \begin_layout Plain Layout
  8712. AUC
  8713. \end_layout
  8714. \end_inset
  8715. values were generated
  8716. \begin_inset CommandInset citation
  8717. LatexCommand cite
  8718. key "Turck2011"
  8719. literal "false"
  8720. \end_inset
  8721. .
  8722. Each normalization was tested on two different sets of training and validation
  8723. samples.
  8724. For internal validation, the 115
  8725. \begin_inset Flex Glossary Term
  8726. status open
  8727. \begin_layout Plain Layout
  8728. TX
  8729. \end_layout
  8730. \end_inset
  8731. and
  8732. \begin_inset Flex Glossary Term
  8733. status open
  8734. \begin_layout Plain Layout
  8735. AR
  8736. \end_layout
  8737. \end_inset
  8738. arrays in the internal set were split at random into two equal sized sets,
  8739. one for training and one for validation, each containing the same numbers
  8740. of
  8741. \begin_inset Flex Glossary Term
  8742. status open
  8743. \begin_layout Plain Layout
  8744. TX
  8745. \end_layout
  8746. \end_inset
  8747. and
  8748. \begin_inset Flex Glossary Term
  8749. status open
  8750. \begin_layout Plain Layout
  8751. AR
  8752. \end_layout
  8753. \end_inset
  8754. samples as the other set.
  8755. For external validation, the full set of 115
  8756. \begin_inset Flex Glossary Term
  8757. status open
  8758. \begin_layout Plain Layout
  8759. TX
  8760. \end_layout
  8761. \end_inset
  8762. and
  8763. \begin_inset Flex Glossary Term
  8764. status open
  8765. \begin_layout Plain Layout
  8766. AR
  8767. \end_layout
  8768. \end_inset
  8769. samples were used as a training set, and the 75 external
  8770. \begin_inset Flex Glossary Term
  8771. status open
  8772. \begin_layout Plain Layout
  8773. TX
  8774. \end_layout
  8775. \end_inset
  8776. and
  8777. \begin_inset Flex Glossary Term
  8778. status open
  8779. \begin_layout Plain Layout
  8780. AR
  8781. \end_layout
  8782. \end_inset
  8783. samples were used as the validation set.
  8784. Thus, 2
  8785. \begin_inset Flex Glossary Term
  8786. status open
  8787. \begin_layout Plain Layout
  8788. ROC
  8789. \end_layout
  8790. \end_inset
  8791. curves and
  8792. \begin_inset Flex Glossary Term
  8793. status open
  8794. \begin_layout Plain Layout
  8795. AUC
  8796. \end_layout
  8797. \end_inset
  8798. values were generated for each normalization method: one internal and one
  8799. external.
  8800. Because the external validation set contains no
  8801. \begin_inset Flex Glossary Term
  8802. status open
  8803. \begin_layout Plain Layout
  8804. ADNR
  8805. \end_layout
  8806. \end_inset
  8807. samples, only classification of
  8808. \begin_inset Flex Glossary Term
  8809. status open
  8810. \begin_layout Plain Layout
  8811. TX
  8812. \end_layout
  8813. \end_inset
  8814. and
  8815. \begin_inset Flex Glossary Term
  8816. status open
  8817. \begin_layout Plain Layout
  8818. AR
  8819. \end_layout
  8820. \end_inset
  8821. samples was considered.
  8822. The
  8823. \begin_inset Flex Glossary Term
  8824. status open
  8825. \begin_layout Plain Layout
  8826. ADNR
  8827. \end_layout
  8828. \end_inset
  8829. samples were included during normalization but excluded from all classifier
  8830. training and validation.
  8831. This ensures that the performance on internal and external validation sets
  8832. is directly comparable, since both are performing the same task: distinguishing
  8833. \begin_inset Flex Glossary Term
  8834. status open
  8835. \begin_layout Plain Layout
  8836. TX
  8837. \end_layout
  8838. \end_inset
  8839. from
  8840. \begin_inset Flex Glossary Term
  8841. status open
  8842. \begin_layout Plain Layout
  8843. AR
  8844. \end_layout
  8845. \end_inset
  8846. .
  8847. \end_layout
  8848. \begin_layout Standard
  8849. \begin_inset Flex TODO Note (inline)
  8850. status open
  8851. \begin_layout Plain Layout
  8852. Summarize the get.best.threshold algorithm for PAM threshold selection, or
  8853. just put the code online?
  8854. \end_layout
  8855. \end_inset
  8856. \end_layout
  8857. \begin_layout Standard
  8858. Six different normalization strategies were evaluated.
  8859. First, 2 well-known non-single-channel normalization methods were considered:
  8860. \begin_inset Flex Glossary Term
  8861. status open
  8862. \begin_layout Plain Layout
  8863. RMA
  8864. \end_layout
  8865. \end_inset
  8866. and dChip
  8867. \begin_inset CommandInset citation
  8868. LatexCommand cite
  8869. key "Li2001,Irizarry2003a"
  8870. literal "false"
  8871. \end_inset
  8872. .
  8873. Since
  8874. \begin_inset Flex Glossary Term
  8875. status open
  8876. \begin_layout Plain Layout
  8877. RMA
  8878. \end_layout
  8879. \end_inset
  8880. produces expression values on a
  8881. \begin_inset Formula $\log_{2}$
  8882. \end_inset
  8883. scale and dChip does not, the values from dChip were
  8884. \begin_inset Formula $\log_{2}$
  8885. \end_inset
  8886. transformed after normalization.
  8887. Next,
  8888. \begin_inset Flex Glossary Term
  8889. status open
  8890. \begin_layout Plain Layout
  8891. RMA
  8892. \end_layout
  8893. \end_inset
  8894. and dChip followed by
  8895. \begin_inset Flex Glossary Term
  8896. status open
  8897. \begin_layout Plain Layout
  8898. GRSN
  8899. \end_layout
  8900. \end_inset
  8901. were tested
  8902. \begin_inset CommandInset citation
  8903. LatexCommand cite
  8904. key "Pelz2008"
  8905. literal "false"
  8906. \end_inset
  8907. .
  8908. Post-processing with
  8909. \begin_inset Flex Glossary Term
  8910. status open
  8911. \begin_layout Plain Layout
  8912. GRSN
  8913. \end_layout
  8914. \end_inset
  8915. does not turn
  8916. \begin_inset Flex Glossary Term
  8917. status open
  8918. \begin_layout Plain Layout
  8919. RMA
  8920. \end_layout
  8921. \end_inset
  8922. or dChip into single-channel methods, but it may help mitigate batch effects
  8923. and is therefore useful as a benchmark.
  8924. Lastly, the two single-channel normalization methods,
  8925. \begin_inset Flex Glossary Term
  8926. status open
  8927. \begin_layout Plain Layout
  8928. fRMA
  8929. \end_layout
  8930. \end_inset
  8931. and
  8932. \begin_inset Flex Glossary Term
  8933. status open
  8934. \begin_layout Plain Layout
  8935. SCAN
  8936. \end_layout
  8937. \end_inset
  8938. , were tested
  8939. \begin_inset CommandInset citation
  8940. LatexCommand cite
  8941. key "McCall2010,Piccolo2012"
  8942. literal "false"
  8943. \end_inset
  8944. .
  8945. When evaluating internal validation performance, only the 157 internal
  8946. samples were normalized; when evaluating external validation performance,
  8947. all 157 internal samples and 75 external samples were normalized together.
  8948. \end_layout
  8949. \begin_layout Standard
  8950. For demonstrating the problem with separate normalization of training and
  8951. validation data, one additional normalization was performed: the internal
  8952. and external sets were each normalized separately using
  8953. \begin_inset Flex Glossary Term
  8954. status open
  8955. \begin_layout Plain Layout
  8956. RMA
  8957. \end_layout
  8958. \end_inset
  8959. , and the normalized data for each set were combined into a single set with
  8960. no further attempts at normalizing between the two sets.
  8961. This represents approximately how
  8962. \begin_inset Flex Glossary Term
  8963. status open
  8964. \begin_layout Plain Layout
  8965. RMA
  8966. \end_layout
  8967. \end_inset
  8968. would have to be used in a clinical setting, where the samples to be classified
  8969. are not available at the time the classifier is trained.
  8970. \end_layout
  8971. \begin_layout Subsection
  8972. Generating custom fRMA vectors for hthgu133pluspm array platform
  8973. \end_layout
  8974. \begin_layout Standard
  8975. In order to enable
  8976. \begin_inset Flex Glossary Term
  8977. status open
  8978. \begin_layout Plain Layout
  8979. fRMA
  8980. \end_layout
  8981. \end_inset
  8982. normalization for the hthgu133pluspm array platform, custom
  8983. \begin_inset Flex Glossary Term
  8984. status open
  8985. \begin_layout Plain Layout
  8986. fRMA
  8987. \end_layout
  8988. \end_inset
  8989. normalization vectors were trained using the
  8990. \begin_inset Flex Code
  8991. status open
  8992. \begin_layout Plain Layout
  8993. frmaTools
  8994. \end_layout
  8995. \end_inset
  8996. package
  8997. \begin_inset CommandInset citation
  8998. LatexCommand cite
  8999. key "McCall2011"
  9000. literal "false"
  9001. \end_inset
  9002. .
  9003. Separate vectors were created for two types of samples: kidney graft biopsy
  9004. samples and blood samples from graft recipients.
  9005. For training, 341 kidney biopsy samples from 2 data sets and 965 blood
  9006. samples from 5 data sets were used as the reference set.
  9007. Arrays were groups into batches based on unique combinations of sample
  9008. type (blood or biopsy), diagnosis (TX, AR, etc.), data set, and scan date.
  9009. Thus, each batch represents arrays of the same kind that were run together
  9010. on the same day.
  9011. For estimating the probe inverse variance weights, frmaTools requires equal-siz
  9012. ed batches, which means a batch size must be chosen, and then batches smaller
  9013. than that size must be ignored, while batches larger than the chosen size
  9014. must be downsampled.
  9015. This downsampling is performed randomly, so the sampling process is repeated
  9016. 5 times and the resulting normalizations are compared to each other.
  9017. \end_layout
  9018. \begin_layout Standard
  9019. To evaluate the consistency of the generated normalization vectors, the
  9020. 5
  9021. \begin_inset Flex Glossary Term
  9022. status open
  9023. \begin_layout Plain Layout
  9024. fRMA
  9025. \end_layout
  9026. \end_inset
  9027. vector sets generated from 5 random batch samplings were each used to normalize
  9028. the same 20 randomly selected samples from each tissue.
  9029. Then the normalized expression values for each probe on each array were
  9030. compared across all normalizations.
  9031. Each
  9032. \begin_inset Flex Glossary Term
  9033. status open
  9034. \begin_layout Plain Layout
  9035. fRMA
  9036. \end_layout
  9037. \end_inset
  9038. normalization was also compared against the normalized expression values
  9039. obtained by normalizing the same 20 samples with ordinary
  9040. \begin_inset Flex Glossary Term
  9041. status open
  9042. \begin_layout Plain Layout
  9043. RMA
  9044. \end_layout
  9045. \end_inset
  9046. .
  9047. \end_layout
  9048. \begin_layout Subsection
  9049. Modeling methylation array M-value heteroskedasticity with a modified voom
  9050. implementation
  9051. \end_layout
  9052. \begin_layout Standard
  9053. \begin_inset Flex TODO Note (inline)
  9054. status open
  9055. \begin_layout Plain Layout
  9056. Put code on Github and reference it.
  9057. \end_layout
  9058. \end_inset
  9059. \end_layout
  9060. \begin_layout Standard
  9061. To investigate the whether DNA methylation could be used to distinguish
  9062. between healthy and dysfunctional transplants, a data set of 78 Illumina
  9063. 450k methylation arrays from human kidney graft biopsies was analyzed for
  9064. differential methylation between 4 transplant statuses:
  9065. \begin_inset Flex Glossary Term
  9066. status open
  9067. \begin_layout Plain Layout
  9068. TX
  9069. \end_layout
  9070. \end_inset
  9071. , transplants undergoing
  9072. \begin_inset Flex Glossary Term
  9073. status open
  9074. \begin_layout Plain Layout
  9075. AR
  9076. \end_layout
  9077. \end_inset
  9078. ,
  9079. \begin_inset Flex Glossary Term
  9080. status open
  9081. \begin_layout Plain Layout
  9082. ADNR
  9083. \end_layout
  9084. \end_inset
  9085. , and
  9086. \begin_inset Flex Glossary Term
  9087. status open
  9088. \begin_layout Plain Layout
  9089. CAN
  9090. \end_layout
  9091. \end_inset
  9092. .
  9093. The data consisted of 33 TX, 9 AR, 8 ADNR, and 28 CAN samples.
  9094. The uneven group sizes are a result of taking the biopsy samples before
  9095. the eventual fate of the transplant was known.
  9096. Each sample was additionally annotated with a donor
  9097. \begin_inset Flex Glossary Term
  9098. status open
  9099. \begin_layout Plain Layout
  9100. ID
  9101. \end_layout
  9102. \end_inset
  9103. (anonymized), sex, age, ethnicity, creatinine level, and diabetes diagnosis
  9104. (all samples in this data set came from patients with either
  9105. \begin_inset Flex Glossary Term
  9106. status open
  9107. \begin_layout Plain Layout
  9108. T1D
  9109. \end_layout
  9110. \end_inset
  9111. or
  9112. \begin_inset Flex Glossary Term
  9113. status open
  9114. \begin_layout Plain Layout
  9115. T2D
  9116. \end_layout
  9117. \end_inset
  9118. ).
  9119. \end_layout
  9120. \begin_layout Standard
  9121. The intensity data were first normalized using
  9122. \begin_inset Flex Glossary Term
  9123. status open
  9124. \begin_layout Plain Layout
  9125. SWAN
  9126. \end_layout
  9127. \end_inset
  9128. \begin_inset CommandInset citation
  9129. LatexCommand cite
  9130. key "Maksimovic2012"
  9131. literal "false"
  9132. \end_inset
  9133. , then converted to intensity ratios (beta values)
  9134. \begin_inset CommandInset citation
  9135. LatexCommand cite
  9136. key "Aryee2014"
  9137. literal "false"
  9138. \end_inset
  9139. .
  9140. Any probes binding to loci that overlapped annotated SNPs were dropped,
  9141. and the annotated sex of each sample was verified against the sex inferred
  9142. from the ratio of median probe intensities for the X and Y chromosomes.
  9143. Then, the ratios were transformed to
  9144. \begin_inset Flex Glossary Term (pl)
  9145. status open
  9146. \begin_layout Plain Layout
  9147. M-value
  9148. \end_layout
  9149. \end_inset
  9150. .
  9151. \end_layout
  9152. \begin_layout Standard
  9153. \begin_inset Float table
  9154. wide false
  9155. sideways false
  9156. status collapsed
  9157. \begin_layout Plain Layout
  9158. \align center
  9159. \begin_inset Tabular
  9160. <lyxtabular version="3" rows="4" columns="6">
  9161. <features tabularvalignment="middle">
  9162. <column alignment="center" valignment="top">
  9163. <column alignment="center" valignment="top">
  9164. <column alignment="center" valignment="top">
  9165. <column alignment="center" valignment="top">
  9166. <column alignment="center" valignment="top">
  9167. <column alignment="center" valignment="top">
  9168. <row>
  9169. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  9170. \begin_inset Text
  9171. \begin_layout Plain Layout
  9172. Analysis
  9173. \end_layout
  9174. \end_inset
  9175. </cell>
  9176. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  9177. \begin_inset Text
  9178. \begin_layout Plain Layout
  9179. random effect
  9180. \end_layout
  9181. \end_inset
  9182. </cell>
  9183. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  9184. \begin_inset Text
  9185. \begin_layout Plain Layout
  9186. eBayes
  9187. \end_layout
  9188. \end_inset
  9189. </cell>
  9190. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  9191. \begin_inset Text
  9192. \begin_layout Plain Layout
  9193. SVA
  9194. \end_layout
  9195. \end_inset
  9196. </cell>
  9197. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  9198. \begin_inset Text
  9199. \begin_layout Plain Layout
  9200. weights
  9201. \end_layout
  9202. \end_inset
  9203. </cell>
  9204. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" rightline="true" usebox="none">
  9205. \begin_inset Text
  9206. \begin_layout Plain Layout
  9207. voom
  9208. \end_layout
  9209. \end_inset
  9210. </cell>
  9211. </row>
  9212. <row>
  9213. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  9214. \begin_inset Text
  9215. \begin_layout Plain Layout
  9216. A
  9217. \end_layout
  9218. \end_inset
  9219. </cell>
  9220. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  9221. \begin_inset Text
  9222. \begin_layout Plain Layout
  9223. Yes
  9224. \end_layout
  9225. \end_inset
  9226. </cell>
  9227. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  9228. \begin_inset Text
  9229. \begin_layout Plain Layout
  9230. Yes
  9231. \end_layout
  9232. \end_inset
  9233. </cell>
  9234. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  9235. \begin_inset Text
  9236. \begin_layout Plain Layout
  9237. No
  9238. \end_layout
  9239. \end_inset
  9240. </cell>
  9241. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  9242. \begin_inset Text
  9243. \begin_layout Plain Layout
  9244. No
  9245. \end_layout
  9246. \end_inset
  9247. </cell>
  9248. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  9249. \begin_inset Text
  9250. \begin_layout Plain Layout
  9251. No
  9252. \end_layout
  9253. \end_inset
  9254. </cell>
  9255. </row>
  9256. <row>
  9257. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  9258. \begin_inset Text
  9259. \begin_layout Plain Layout
  9260. B
  9261. \end_layout
  9262. \end_inset
  9263. </cell>
  9264. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  9265. \begin_inset Text
  9266. \begin_layout Plain Layout
  9267. Yes
  9268. \end_layout
  9269. \end_inset
  9270. </cell>
  9271. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  9272. \begin_inset Text
  9273. \begin_layout Plain Layout
  9274. Yes
  9275. \end_layout
  9276. \end_inset
  9277. </cell>
  9278. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  9279. \begin_inset Text
  9280. \begin_layout Plain Layout
  9281. Yes
  9282. \end_layout
  9283. \end_inset
  9284. </cell>
  9285. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  9286. \begin_inset Text
  9287. \begin_layout Plain Layout
  9288. Yes
  9289. \end_layout
  9290. \end_inset
  9291. </cell>
  9292. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  9293. \begin_inset Text
  9294. \begin_layout Plain Layout
  9295. No
  9296. \end_layout
  9297. \end_inset
  9298. </cell>
  9299. </row>
  9300. <row>
  9301. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  9302. \begin_inset Text
  9303. \begin_layout Plain Layout
  9304. C
  9305. \end_layout
  9306. \end_inset
  9307. </cell>
  9308. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  9309. \begin_inset Text
  9310. \begin_layout Plain Layout
  9311. Yes
  9312. \end_layout
  9313. \end_inset
  9314. </cell>
  9315. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  9316. \begin_inset Text
  9317. \begin_layout Plain Layout
  9318. Yes
  9319. \end_layout
  9320. \end_inset
  9321. </cell>
  9322. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  9323. \begin_inset Text
  9324. \begin_layout Plain Layout
  9325. Yes
  9326. \end_layout
  9327. \end_inset
  9328. </cell>
  9329. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  9330. \begin_inset Text
  9331. \begin_layout Plain Layout
  9332. Yes
  9333. \end_layout
  9334. \end_inset
  9335. </cell>
  9336. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" rightline="true" usebox="none">
  9337. \begin_inset Text
  9338. \begin_layout Plain Layout
  9339. Yes
  9340. \end_layout
  9341. \end_inset
  9342. </cell>
  9343. </row>
  9344. </lyxtabular>
  9345. \end_inset
  9346. \end_layout
  9347. \begin_layout Plain Layout
  9348. \begin_inset Caption Standard
  9349. \begin_layout Plain Layout
  9350. \begin_inset Argument 1
  9351. status collapsed
  9352. \begin_layout Plain Layout
  9353. Summary of analysis variants for methylation array data.
  9354. \end_layout
  9355. \end_inset
  9356. \begin_inset CommandInset label
  9357. LatexCommand label
  9358. name "tab:Summary-of-meth-analysis"
  9359. \end_inset
  9360. \series bold
  9361. Summary of analysis variants for methylation array data.
  9362. \series default
  9363. Each analysis included a different set of steps to adjust or account for
  9364. various systematic features of the data.
  9365. Random effect: The model included a random effect accounting for correlation
  9366. between samples from the same patient
  9367. \begin_inset CommandInset citation
  9368. LatexCommand cite
  9369. key "Smyth2005a"
  9370. literal "false"
  9371. \end_inset
  9372. ; eBayes: Empirical bayes squeezing of per-probe variances toward the mean-varia
  9373. nce trend
  9374. \begin_inset CommandInset citation
  9375. LatexCommand cite
  9376. key "Ritchie2015"
  9377. literal "false"
  9378. \end_inset
  9379. ; SVA: Surrogate variable analysis to account for unobserved confounders
  9380. \begin_inset CommandInset citation
  9381. LatexCommand cite
  9382. key "Leek2007"
  9383. literal "false"
  9384. \end_inset
  9385. ; Weights: Estimate sample weights to account for differences in sample
  9386. quality
  9387. \begin_inset CommandInset citation
  9388. LatexCommand cite
  9389. key "Liu2015,Ritchie2006"
  9390. literal "false"
  9391. \end_inset
  9392. ; voom: Use mean-variance trend to assign individual sample weights
  9393. \begin_inset CommandInset citation
  9394. LatexCommand cite
  9395. key "Law2013"
  9396. literal "false"
  9397. \end_inset
  9398. .
  9399. See the text for a more detailed explanation of each step.
  9400. \end_layout
  9401. \end_inset
  9402. \end_layout
  9403. \end_inset
  9404. \end_layout
  9405. \begin_layout Standard
  9406. From the
  9407. \begin_inset Flex Glossary Term (pl)
  9408. status open
  9409. \begin_layout Plain Layout
  9410. M-value
  9411. \end_layout
  9412. \end_inset
  9413. , a series of parallel analyses was performed, each adding additional steps
  9414. into the model fit to accommodate a feature of the data (see Table
  9415. \begin_inset CommandInset ref
  9416. LatexCommand ref
  9417. reference "tab:Summary-of-meth-analysis"
  9418. plural "false"
  9419. caps "false"
  9420. noprefix "false"
  9421. \end_inset
  9422. ).
  9423. For analysis A, a
  9424. \begin_inset Quotes eld
  9425. \end_inset
  9426. basic
  9427. \begin_inset Quotes erd
  9428. \end_inset
  9429. linear modeling analysis was performed, compensating for known confounders
  9430. by including terms for the factor of interest (transplant status) as well
  9431. as the known biological confounders: sex, age, ethnicity, and diabetes.
  9432. Since some samples came from the same patients at different times, the
  9433. intra-patient correlation was modeled as a random effect, estimating a
  9434. shared correlation value across all probes
  9435. \begin_inset CommandInset citation
  9436. LatexCommand cite
  9437. key "Smyth2005a"
  9438. literal "false"
  9439. \end_inset
  9440. .
  9441. Then the linear model was fit, and the variance was modeled using empirical
  9442. Bayes squeezing toward the mean-variance trend
  9443. \begin_inset CommandInset citation
  9444. LatexCommand cite
  9445. key "Ritchie2015"
  9446. literal "false"
  9447. \end_inset
  9448. .
  9449. Finally, t-tests or F-tests were performed as appropriate for each test:
  9450. t-tests for single contrasts, and F-tests for multiple contrasts.
  9451. P-values were corrected for multiple testing using the
  9452. \begin_inset Flex Glossary Term
  9453. status open
  9454. \begin_layout Plain Layout
  9455. BH
  9456. \end_layout
  9457. \end_inset
  9458. procedure for
  9459. \begin_inset Flex Glossary Term
  9460. status open
  9461. \begin_layout Plain Layout
  9462. FDR
  9463. \end_layout
  9464. \end_inset
  9465. control
  9466. \begin_inset CommandInset citation
  9467. LatexCommand cite
  9468. key "Benjamini1995"
  9469. literal "false"
  9470. \end_inset
  9471. .
  9472. \end_layout
  9473. \begin_layout Standard
  9474. For the analysis B,
  9475. \begin_inset Flex Glossary Term
  9476. status open
  9477. \begin_layout Plain Layout
  9478. SVA
  9479. \end_layout
  9480. \end_inset
  9481. was used to infer additional unobserved sources of heterogeneity in the
  9482. data
  9483. \begin_inset CommandInset citation
  9484. LatexCommand cite
  9485. key "Leek2007"
  9486. literal "false"
  9487. \end_inset
  9488. .
  9489. These surrogate variables were added to the design matrix before fitting
  9490. the linear model.
  9491. In addition, sample quality weights were estimated from the data and used
  9492. during linear modeling to down-weight the contribution of highly variable
  9493. arrays while increasing the weight to arrays with lower variability
  9494. \begin_inset CommandInset citation
  9495. LatexCommand cite
  9496. key "Ritchie2006"
  9497. literal "false"
  9498. \end_inset
  9499. .
  9500. The remainder of the analysis proceeded as in analysis A.
  9501. For analysis C, the voom method was adapted to run on methylation array
  9502. data and used to model and correct for the mean-variance trend using individual
  9503. observation weights
  9504. \begin_inset CommandInset citation
  9505. LatexCommand cite
  9506. key "Law2013"
  9507. literal "false"
  9508. \end_inset
  9509. , which were combined with the sample weights
  9510. \begin_inset CommandInset citation
  9511. LatexCommand cite
  9512. key "Liu2015,Ritchie2006"
  9513. literal "false"
  9514. \end_inset
  9515. .
  9516. Each time weights were used, they were estimated once before estimating
  9517. the random effect correlation value, and then the weights were re-estimated
  9518. taking the random effect into account.
  9519. The remainder of the analysis proceeded as in analysis B.
  9520. \end_layout
  9521. \begin_layout Section
  9522. Results
  9523. \end_layout
  9524. \begin_layout Standard
  9525. \begin_inset Flex TODO Note (inline)
  9526. status open
  9527. \begin_layout Plain Layout
  9528. Improve subsection titles in this section.
  9529. \end_layout
  9530. \end_inset
  9531. \end_layout
  9532. \begin_layout Standard
  9533. \begin_inset Flex TODO Note (inline)
  9534. status open
  9535. \begin_layout Plain Layout
  9536. Reconsider subsection organization?
  9537. \end_layout
  9538. \end_inset
  9539. \end_layout
  9540. \begin_layout Subsection
  9541. Separate normalization with RMA introduces unwanted biases in classification
  9542. \end_layout
  9543. \begin_layout Standard
  9544. To demonstrate the problem with non-single-channel normalization methods,
  9545. we considered the problem of training a classifier to distinguish
  9546. \begin_inset Flex Glossary Term
  9547. status open
  9548. \begin_layout Plain Layout
  9549. TX
  9550. \end_layout
  9551. \end_inset
  9552. from
  9553. \begin_inset Flex Glossary Term
  9554. status open
  9555. \begin_layout Plain Layout
  9556. AR
  9557. \end_layout
  9558. \end_inset
  9559. using the samples from the internal set as training data, evaluating performanc
  9560. e on the external set.
  9561. First, training and evaluation were performed after normalizing all array
  9562. samples together as a single set using
  9563. \begin_inset Flex Glossary Term
  9564. status open
  9565. \begin_layout Plain Layout
  9566. RMA
  9567. \end_layout
  9568. \end_inset
  9569. , and second, the internal samples were normalized separately from the external
  9570. samples and the training and evaluation were repeated.
  9571. For each sample in the validation set, the classifier probabilities from
  9572. both classifiers were plotted against each other (Fig.
  9573. \begin_inset CommandInset ref
  9574. LatexCommand ref
  9575. reference "fig:Classifier-probabilities-RMA"
  9576. plural "false"
  9577. caps "false"
  9578. noprefix "false"
  9579. \end_inset
  9580. ).
  9581. As expected, separate normalization biases the classifier probabilities,
  9582. resulting in several misclassifications.
  9583. In this case, the bias from separate normalization causes the classifier
  9584. to assign a lower probability of
  9585. \begin_inset Flex Glossary Term
  9586. status open
  9587. \begin_layout Plain Layout
  9588. AR
  9589. \end_layout
  9590. \end_inset
  9591. to every sample.
  9592. \end_layout
  9593. \begin_layout Standard
  9594. \begin_inset Float figure
  9595. wide false
  9596. sideways false
  9597. status collapsed
  9598. \begin_layout Plain Layout
  9599. \align center
  9600. \begin_inset Graphics
  9601. filename graphics/PAM/predplot.pdf
  9602. lyxscale 50
  9603. width 60col%
  9604. groupId colwidth
  9605. \end_inset
  9606. \end_layout
  9607. \begin_layout Plain Layout
  9608. \begin_inset Caption Standard
  9609. \begin_layout Plain Layout
  9610. \begin_inset Argument 1
  9611. status collapsed
  9612. \begin_layout Plain Layout
  9613. Classifier probabilities on validation samples when normalized with RMA
  9614. together vs.
  9615. separately.
  9616. \end_layout
  9617. \end_inset
  9618. \begin_inset CommandInset label
  9619. LatexCommand label
  9620. name "fig:Classifier-probabilities-RMA"
  9621. \end_inset
  9622. \series bold
  9623. Classifier probabilities on validation samples when normalized with RMA
  9624. together vs.
  9625. separately.
  9626. \series default
  9627. The PAM classifier algorithm was trained on the training set of arrays to
  9628. distinguish AR from TX and then used to assign class probabilities to the
  9629. validation set.
  9630. The process was performed after normalizing all samples together and after
  9631. normalizing the training and test sets separately, and the class probabilities
  9632. assigned to each sample in the validation set were plotted against each
  9633. other.
  9634. Each axis indicates the posterior probability of AR assigned to a sample
  9635. by the classifier in the specified analysis.
  9636. The color of each point indicates the true classification of that sample.
  9637. \end_layout
  9638. \end_inset
  9639. \end_layout
  9640. \end_inset
  9641. \end_layout
  9642. \begin_layout Subsection
  9643. fRMA and SCAN maintain classification performance while eliminating dependence
  9644. on normalization strategy
  9645. \end_layout
  9646. \begin_layout Standard
  9647. For internal validation, the 6 methods' AUC values ranged from 0.816 to 0.891,
  9648. as shown in Table
  9649. \begin_inset CommandInset ref
  9650. LatexCommand ref
  9651. reference "tab:AUC-PAM"
  9652. plural "false"
  9653. caps "false"
  9654. noprefix "false"
  9655. \end_inset
  9656. .
  9657. Among the non-single-channel normalizations, dChip outperformed
  9658. \begin_inset Flex Glossary Term
  9659. status open
  9660. \begin_layout Plain Layout
  9661. RMA
  9662. \end_layout
  9663. \end_inset
  9664. , while
  9665. \begin_inset Flex Glossary Term
  9666. status open
  9667. \begin_layout Plain Layout
  9668. GRSN
  9669. \end_layout
  9670. \end_inset
  9671. reduced the
  9672. \begin_inset Flex Glossary Term
  9673. status open
  9674. \begin_layout Plain Layout
  9675. AUC
  9676. \end_layout
  9677. \end_inset
  9678. values for both dChip and
  9679. \begin_inset Flex Glossary Term
  9680. status open
  9681. \begin_layout Plain Layout
  9682. RMA
  9683. \end_layout
  9684. \end_inset
  9685. .
  9686. Both single-channel methods,
  9687. \begin_inset Flex Glossary Term
  9688. status open
  9689. \begin_layout Plain Layout
  9690. fRMA
  9691. \end_layout
  9692. \end_inset
  9693. and
  9694. \begin_inset Flex Glossary Term
  9695. status open
  9696. \begin_layout Plain Layout
  9697. SCAN
  9698. \end_layout
  9699. \end_inset
  9700. , slightly outperformed
  9701. \begin_inset Flex Glossary Term
  9702. status open
  9703. \begin_layout Plain Layout
  9704. RMA
  9705. \end_layout
  9706. \end_inset
  9707. , with
  9708. \begin_inset Flex Glossary Term
  9709. status open
  9710. \begin_layout Plain Layout
  9711. fRMA
  9712. \end_layout
  9713. \end_inset
  9714. ahead of
  9715. \begin_inset Flex Glossary Term
  9716. status open
  9717. \begin_layout Plain Layout
  9718. SCAN
  9719. \end_layout
  9720. \end_inset
  9721. .
  9722. However, the difference between
  9723. \begin_inset Flex Glossary Term
  9724. status open
  9725. \begin_layout Plain Layout
  9726. RMA
  9727. \end_layout
  9728. \end_inset
  9729. and
  9730. \begin_inset Flex Glossary Term
  9731. status open
  9732. \begin_layout Plain Layout
  9733. fRMA
  9734. \end_layout
  9735. \end_inset
  9736. is still quite small.
  9737. Figure
  9738. \begin_inset CommandInset ref
  9739. LatexCommand ref
  9740. reference "fig:ROC-PAM-int"
  9741. plural "false"
  9742. caps "false"
  9743. noprefix "false"
  9744. \end_inset
  9745. shows that the
  9746. \begin_inset Flex Glossary Term
  9747. status open
  9748. \begin_layout Plain Layout
  9749. ROC
  9750. \end_layout
  9751. \end_inset
  9752. curves for
  9753. \begin_inset Flex Glossary Term
  9754. status open
  9755. \begin_layout Plain Layout
  9756. RMA
  9757. \end_layout
  9758. \end_inset
  9759. , dChip, and
  9760. \begin_inset Flex Glossary Term
  9761. status open
  9762. \begin_layout Plain Layout
  9763. fRMA
  9764. \end_layout
  9765. \end_inset
  9766. look very similar and relatively smooth, while both
  9767. \begin_inset Flex Glossary Term
  9768. status open
  9769. \begin_layout Plain Layout
  9770. GRSN
  9771. \end_layout
  9772. \end_inset
  9773. curves and the curve for
  9774. \begin_inset Flex Glossary Term
  9775. status open
  9776. \begin_layout Plain Layout
  9777. SCAN
  9778. \end_layout
  9779. \end_inset
  9780. have a more jagged appearance.
  9781. \end_layout
  9782. \begin_layout Standard
  9783. \begin_inset Float figure
  9784. wide false
  9785. sideways false
  9786. status collapsed
  9787. \begin_layout Plain Layout
  9788. \align center
  9789. \begin_inset Float figure
  9790. placement tb
  9791. wide false
  9792. sideways false
  9793. status open
  9794. \begin_layout Plain Layout
  9795. \align center
  9796. \begin_inset Graphics
  9797. filename graphics/PAM/ROC-TXvsAR-internal.pdf
  9798. lyxscale 50
  9799. height 40theight%
  9800. groupId roc-pam
  9801. \end_inset
  9802. \end_layout
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  9804. \begin_inset Caption Standard
  9805. \begin_layout Plain Layout
  9806. \begin_inset CommandInset label
  9807. LatexCommand label
  9808. name "fig:ROC-PAM-int"
  9809. \end_inset
  9810. ROC curves for PAM on internal validation data
  9811. \end_layout
  9812. \end_inset
  9813. \end_layout
  9814. \end_inset
  9815. \end_layout
  9816. \begin_layout Plain Layout
  9817. \align center
  9818. \begin_inset Float figure
  9819. placement tb
  9820. wide false
  9821. sideways false
  9822. status open
  9823. \begin_layout Plain Layout
  9824. \align center
  9825. \begin_inset Graphics
  9826. filename graphics/PAM/ROC-TXvsAR-external.pdf
  9827. lyxscale 50
  9828. height 40theight%
  9829. groupId roc-pam
  9830. \end_inset
  9831. \end_layout
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  9833. \begin_inset Caption Standard
  9834. \begin_layout Plain Layout
  9835. \begin_inset CommandInset label
  9836. LatexCommand label
  9837. name "fig:ROC-PAM-ext"
  9838. \end_inset
  9839. ROC curves for PAM on external validation data
  9840. \end_layout
  9841. \end_inset
  9842. \end_layout
  9843. \end_inset
  9844. \end_layout
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  9846. \begin_inset Caption Standard
  9847. \begin_layout Plain Layout
  9848. \begin_inset Argument 1
  9849. status collapsed
  9850. \begin_layout Plain Layout
  9851. ROC curves for PAM using different normalization strategies.
  9852. \end_layout
  9853. \end_inset
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  9855. LatexCommand label
  9856. name "fig:ROC-PAM-main"
  9857. \end_inset
  9858. \series bold
  9859. ROC curves for PAM using different normalization strategies.
  9860. \series default
  9861. ROC curves were generated for PAM classification of AR vs TX after 6 different
  9862. normalization strategies applied to the same data sets.
  9863. Only fRMA and SCAN are single-channel normalizations.
  9864. The other normalizations are for comparison.
  9865. \end_layout
  9866. \end_inset
  9867. \end_layout
  9868. \end_inset
  9869. \end_layout
  9870. \begin_layout Standard
  9871. \begin_inset Float table
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  9881. <column alignment="center" valignment="top">
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  10017. \xout off
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  10020. \noun off
  10021. \color none
  10022. dChip
  10023. \end_layout
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  10026. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
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  10087. \color none
  10088. RMA + GRSN
  10089. \end_layout
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  10314. \end_inset
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  10316. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" rightline="true" usebox="none">
  10317. \begin_inset Text
  10318. \begin_layout Plain Layout
  10319. \family roman
  10320. \series medium
  10321. \shape up
  10322. \size normal
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  10325. \strikeout off
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  10331. 0.689
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  10333. \end_inset
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  10336. </lyxtabular>
  10337. \end_inset
  10338. \end_layout
  10339. \begin_layout Plain Layout
  10340. \begin_inset Caption Standard
  10341. \begin_layout Plain Layout
  10342. \begin_inset Argument 1
  10343. status collapsed
  10344. \begin_layout Plain Layout
  10345. ROC curve AUC values for internal and external validation with 6 different
  10346. normalization strategies.
  10347. \end_layout
  10348. \end_inset
  10349. \begin_inset CommandInset label
  10350. LatexCommand label
  10351. name "tab:AUC-PAM"
  10352. \end_inset
  10353. \series bold
  10354. ROC curve AUC values for internal and external validation with 6 different
  10355. normalization strategies.
  10356. \series default
  10357. These AUC values correspond to the ROC curves in Figure
  10358. \begin_inset CommandInset ref
  10359. LatexCommand ref
  10360. reference "fig:ROC-PAM-main"
  10361. plural "false"
  10362. caps "false"
  10363. noprefix "false"
  10364. \end_inset
  10365. .
  10366. \end_layout
  10367. \end_inset
  10368. \end_layout
  10369. \end_inset
  10370. \end_layout
  10371. \begin_layout Standard
  10372. For external validation, as expected, all the
  10373. \begin_inset Flex Glossary Term
  10374. status open
  10375. \begin_layout Plain Layout
  10376. AUC
  10377. \end_layout
  10378. \end_inset
  10379. values are lower than the internal validations, ranging from 0.642 to 0.750
  10380. (Table
  10381. \begin_inset CommandInset ref
  10382. LatexCommand ref
  10383. reference "tab:AUC-PAM"
  10384. plural "false"
  10385. caps "false"
  10386. noprefix "false"
  10387. \end_inset
  10388. ).
  10389. With or without
  10390. \begin_inset Flex Glossary Term
  10391. status open
  10392. \begin_layout Plain Layout
  10393. GRSN
  10394. \end_layout
  10395. \end_inset
  10396. ,
  10397. \begin_inset Flex Glossary Term
  10398. status open
  10399. \begin_layout Plain Layout
  10400. RMA
  10401. \end_layout
  10402. \end_inset
  10403. shows its dominance over dChip in this more challenging test.
  10404. Unlike in the internal validation,
  10405. \begin_inset Flex Glossary Term
  10406. status open
  10407. \begin_layout Plain Layout
  10408. GRSN
  10409. \end_layout
  10410. \end_inset
  10411. actually improves the classifier performance for
  10412. \begin_inset Flex Glossary Term
  10413. status open
  10414. \begin_layout Plain Layout
  10415. RMA
  10416. \end_layout
  10417. \end_inset
  10418. , although it does not for dChip.
  10419. Once again, both single-channel methods perform about on par with
  10420. \begin_inset Flex Glossary Term
  10421. status open
  10422. \begin_layout Plain Layout
  10423. RMA
  10424. \end_layout
  10425. \end_inset
  10426. , with
  10427. \begin_inset Flex Glossary Term
  10428. status open
  10429. \begin_layout Plain Layout
  10430. fRMA
  10431. \end_layout
  10432. \end_inset
  10433. performing slightly better and
  10434. \begin_inset Flex Glossary Term
  10435. status open
  10436. \begin_layout Plain Layout
  10437. SCAN
  10438. \end_layout
  10439. \end_inset
  10440. performing a bit worse.
  10441. Figure
  10442. \begin_inset CommandInset ref
  10443. LatexCommand ref
  10444. reference "fig:ROC-PAM-ext"
  10445. plural "false"
  10446. caps "false"
  10447. noprefix "false"
  10448. \end_inset
  10449. shows the
  10450. \begin_inset Flex Glossary Term
  10451. status open
  10452. \begin_layout Plain Layout
  10453. ROC
  10454. \end_layout
  10455. \end_inset
  10456. curves for the external validation test.
  10457. As expected, none of them are as clean-looking as the internal validation
  10458. \begin_inset Flex Glossary Term
  10459. status open
  10460. \begin_layout Plain Layout
  10461. ROC
  10462. \end_layout
  10463. \end_inset
  10464. curves.
  10465. The curves for
  10466. \begin_inset Flex Glossary Term
  10467. status open
  10468. \begin_layout Plain Layout
  10469. RMA
  10470. \end_layout
  10471. \end_inset
  10472. , RMA+GRSN, and
  10473. \begin_inset Flex Glossary Term
  10474. status open
  10475. \begin_layout Plain Layout
  10476. fRMA
  10477. \end_layout
  10478. \end_inset
  10479. all look similar, while the other curves look more divergent.
  10480. \end_layout
  10481. \begin_layout Subsection
  10482. fRMA with custom-generated vectors enables single-channel normalization
  10483. on hthgu133pluspm platform
  10484. \end_layout
  10485. \begin_layout Standard
  10486. In order to enable use of
  10487. \begin_inset Flex Glossary Term
  10488. status open
  10489. \begin_layout Plain Layout
  10490. fRMA
  10491. \end_layout
  10492. \end_inset
  10493. to normalize hthgu133pluspm, a custom set of
  10494. \begin_inset Flex Glossary Term
  10495. status open
  10496. \begin_layout Plain Layout
  10497. fRMA
  10498. \end_layout
  10499. \end_inset
  10500. vectors was created.
  10501. First, an appropriate batch size was chosen by looking at the number of
  10502. batches and number of samples included as a function of batch size (Figure
  10503. \begin_inset CommandInset ref
  10504. LatexCommand ref
  10505. reference "fig:frmatools-batch-size"
  10506. plural "false"
  10507. caps "false"
  10508. noprefix "false"
  10509. \end_inset
  10510. ).
  10511. For a given batch size, all batches with fewer samples that the chosen
  10512. size must be ignored during training, while larger batches must be randomly
  10513. downsampled to the chosen size.
  10514. Hence, the number of samples included for a given batch size equals the
  10515. batch size times the number of batches with at least that many samples.
  10516. From Figure
  10517. \begin_inset CommandInset ref
  10518. LatexCommand ref
  10519. reference "fig:batch-size-samples"
  10520. plural "false"
  10521. caps "false"
  10522. noprefix "false"
  10523. \end_inset
  10524. , it is apparent that a batch size of 8 maximizes the number of samples
  10525. included in training.
  10526. Increasing the batch size beyond this causes too many smaller batches to
  10527. be excluded, reducing the total number of samples for both tissue types.
  10528. However, a batch size of 8 is not necessarily optimal.
  10529. The article introducing frmaTools concluded that it was highly advantageous
  10530. to use a smaller batch size in order to include more batches, even at the
  10531. cost of including fewer total samples in training
  10532. \begin_inset CommandInset citation
  10533. LatexCommand cite
  10534. key "McCall2011"
  10535. literal "false"
  10536. \end_inset
  10537. .
  10538. To strike an appropriate balance between more batches and more samples,
  10539. a batch size of 5 was chosen.
  10540. For both blood and biopsy samples, this increased the number of batches
  10541. included by 10, with only a modest reduction in the number of samples compared
  10542. to a batch size of 8.
  10543. With a batch size of 5, 26 batches of biopsy samples and 46 batches of
  10544. blood samples were available.
  10545. \end_layout
  10546. \begin_layout Standard
  10547. \begin_inset Float figure
  10548. wide false
  10549. sideways false
  10550. status collapsed
  10551. \begin_layout Plain Layout
  10552. \align center
  10553. \begin_inset Float figure
  10554. placement tb
  10555. wide false
  10556. sideways false
  10557. status collapsed
  10558. \begin_layout Plain Layout
  10559. \align center
  10560. \begin_inset Graphics
  10561. filename graphics/frma-pax-bx/batchsize_batches.pdf
  10562. lyxscale 50
  10563. height 35theight%
  10564. groupId frmatools-subfig
  10565. \end_inset
  10566. \end_layout
  10567. \begin_layout Plain Layout
  10568. \begin_inset Caption Standard
  10569. \begin_layout Plain Layout
  10570. \begin_inset CommandInset label
  10571. LatexCommand label
  10572. name "fig:batch-size-batches"
  10573. \end_inset
  10574. \series bold
  10575. Number of batches usable in fRMA probe weight learning as a function of
  10576. batch size.
  10577. \end_layout
  10578. \end_inset
  10579. \end_layout
  10580. \end_inset
  10581. \end_layout
  10582. \begin_layout Plain Layout
  10583. \align center
  10584. \begin_inset Float figure
  10585. placement tb
  10586. wide false
  10587. sideways false
  10588. status collapsed
  10589. \begin_layout Plain Layout
  10590. \align center
  10591. \begin_inset Graphics
  10592. filename graphics/frma-pax-bx/batchsize_samples.pdf
  10593. lyxscale 50
  10594. height 35theight%
  10595. groupId frmatools-subfig
  10596. \end_inset
  10597. \end_layout
  10598. \begin_layout Plain Layout
  10599. \begin_inset Caption Standard
  10600. \begin_layout Plain Layout
  10601. \begin_inset CommandInset label
  10602. LatexCommand label
  10603. name "fig:batch-size-samples"
  10604. \end_inset
  10605. \series bold
  10606. Number of samples usable in fRMA probe weight learning as a function of
  10607. batch size.
  10608. \end_layout
  10609. \end_inset
  10610. \end_layout
  10611. \end_inset
  10612. \end_layout
  10613. \begin_layout Plain Layout
  10614. \begin_inset Caption Standard
  10615. \begin_layout Plain Layout
  10616. \begin_inset Argument 1
  10617. status collapsed
  10618. \begin_layout Plain Layout
  10619. Effect of batch size selection on number of batches and number of samples
  10620. included in fRMA probe weight learning.
  10621. \end_layout
  10622. \end_inset
  10623. \begin_inset CommandInset label
  10624. LatexCommand label
  10625. name "fig:frmatools-batch-size"
  10626. \end_inset
  10627. \series bold
  10628. Effect of batch size selection on number of batches and number of samples
  10629. included in fRMA probe weight learning.
  10630. \series default
  10631. For batch sizes ranging from 3 to 15, the number of batches (a) and samples
  10632. (b) included in probe weight training were plotted for biopsy (BX) and
  10633. blood (PAX) samples.
  10634. The selected batch size, 5, is marked with a dotted vertical line.
  10635. \end_layout
  10636. \end_inset
  10637. \end_layout
  10638. \end_inset
  10639. \end_layout
  10640. \begin_layout Standard
  10641. Since
  10642. \begin_inset Flex Glossary Term
  10643. status open
  10644. \begin_layout Plain Layout
  10645. fRMA
  10646. \end_layout
  10647. \end_inset
  10648. training requires equal-size batches, larger batches are downsampled randomly.
  10649. This introduces a nondeterministic step in the generation of normalization
  10650. vectors.
  10651. To show that this randomness does not substantially change the outcome,
  10652. the random downsampling and subsequent vector learning was repeated 5 times,
  10653. with a different random seed each time.
  10654. 20 samples were selected at random as a test set and normalized with each
  10655. of the 5 sets of
  10656. \begin_inset Flex Glossary Term
  10657. status open
  10658. \begin_layout Plain Layout
  10659. fRMA
  10660. \end_layout
  10661. \end_inset
  10662. normalization vectors as well as ordinary RMA, and the normalized expression
  10663. values were compared across normalizations.
  10664. Figure
  10665. \begin_inset CommandInset ref
  10666. LatexCommand ref
  10667. reference "fig:m-bx-violin"
  10668. plural "false"
  10669. caps "false"
  10670. noprefix "false"
  10671. \end_inset
  10672. shows a summary of these comparisons for biopsy samples.
  10673. Comparing RMA to each of the 5
  10674. \begin_inset Flex Glossary Term
  10675. status open
  10676. \begin_layout Plain Layout
  10677. fRMA
  10678. \end_layout
  10679. \end_inset
  10680. normalizations, the distribution of log ratios is somewhat wide, indicating
  10681. that the normalizations disagree on the expression values of a fair number
  10682. of probe sets.
  10683. In contrast, comparisons of
  10684. \begin_inset Flex Glossary Term
  10685. status open
  10686. \begin_layout Plain Layout
  10687. fRMA
  10688. \end_layout
  10689. \end_inset
  10690. against
  10691. \begin_inset Flex Glossary Term
  10692. status open
  10693. \begin_layout Plain Layout
  10694. fRMA
  10695. \end_layout
  10696. \end_inset
  10697. , the vast majority of probe sets have very small log ratios, indicating
  10698. a very high agreement between the normalized values generated by the two
  10699. normalizations.
  10700. This shows that the
  10701. \begin_inset Flex Glossary Term
  10702. status open
  10703. \begin_layout Plain Layout
  10704. fRMA
  10705. \end_layout
  10706. \end_inset
  10707. normalization's behavior is not very sensitive to the random downsampling
  10708. of larger batches during training.
  10709. \end_layout
  10710. \begin_layout Standard
  10711. \begin_inset Float figure
  10712. wide false
  10713. sideways false
  10714. status collapsed
  10715. \begin_layout Plain Layout
  10716. \align center
  10717. \begin_inset Graphics
  10718. filename graphics/frma-pax-bx/M-BX-violin.pdf
  10719. lyxscale 40
  10720. height 90theight%
  10721. groupId m-violin
  10722. \end_inset
  10723. \end_layout
  10724. \begin_layout Plain Layout
  10725. \begin_inset Caption Standard
  10726. \begin_layout Plain Layout
  10727. \begin_inset Argument 1
  10728. status collapsed
  10729. \begin_layout Plain Layout
  10730. Violin plot of log ratios between normalizations for 20 biopsy samples.
  10731. \end_layout
  10732. \end_inset
  10733. \begin_inset CommandInset label
  10734. LatexCommand label
  10735. name "fig:m-bx-violin"
  10736. \end_inset
  10737. \series bold
  10738. Violin plot of log ratios between normalizations for 20 biopsy samples.
  10739. \series default
  10740. Each of 20 randomly selected samples was normalized with RMA and with 5
  10741. different sets of fRMA vectors.
  10742. The distribution of log ratios between normalized expression values, aggregated
  10743. across all 20 arrays, was plotted for each pair of normalizations.
  10744. \end_layout
  10745. \end_inset
  10746. \end_layout
  10747. \end_inset
  10748. \end_layout
  10749. \begin_layout Standard
  10750. \begin_inset Float figure
  10751. wide false
  10752. sideways false
  10753. status collapsed
  10754. \begin_layout Plain Layout
  10755. \align center
  10756. \begin_inset Graphics
  10757. filename graphics/frma-pax-bx/M-PAX-violin.pdf
  10758. lyxscale 40
  10759. height 90theight%
  10760. groupId m-violin
  10761. \end_inset
  10762. \end_layout
  10763. \begin_layout Plain Layout
  10764. \begin_inset Caption Standard
  10765. \begin_layout Plain Layout
  10766. \begin_inset CommandInset label
  10767. LatexCommand label
  10768. name "fig:m-pax-violin"
  10769. \end_inset
  10770. \begin_inset Argument 1
  10771. status open
  10772. \begin_layout Plain Layout
  10773. Violin plot of log ratios between normalizations for 20 blood samples.
  10774. \end_layout
  10775. \end_inset
  10776. \series bold
  10777. Violin plot of log ratios between normalizations for 20 blood samples.
  10778. \series default
  10779. Each of 20 randomly selected samples was normalized with RMA and with 5
  10780. different sets of fRMA vectors.
  10781. The distribution of log ratios between normalized expression values, aggregated
  10782. across all 20 arrays, was plotted for each pair of normalizations.
  10783. \end_layout
  10784. \end_inset
  10785. \end_layout
  10786. \end_inset
  10787. \end_layout
  10788. \begin_layout Standard
  10789. Figure
  10790. \begin_inset CommandInset ref
  10791. LatexCommand ref
  10792. reference "fig:ma-bx-rma-frma"
  10793. plural "false"
  10794. caps "false"
  10795. noprefix "false"
  10796. \end_inset
  10797. shows an MA plot of the RMA-normalized values against the fRMA-normalized
  10798. values for the same probe sets and arrays, corresponding to the first row
  10799. of Figure
  10800. \begin_inset CommandInset ref
  10801. LatexCommand ref
  10802. reference "fig:m-bx-violin"
  10803. plural "false"
  10804. caps "false"
  10805. noprefix "false"
  10806. \end_inset
  10807. .
  10808. This MA plot shows that not only is there a wide distribution of
  10809. \begin_inset Flex Glossary Term (pl)
  10810. status open
  10811. \begin_layout Plain Layout
  10812. M-value
  10813. \end_layout
  10814. \end_inset
  10815. , but the trend of
  10816. \begin_inset Flex Glossary Term (pl)
  10817. status open
  10818. \begin_layout Plain Layout
  10819. M-value
  10820. \end_layout
  10821. \end_inset
  10822. is dependent on the average normalized intensity.
  10823. This is expected, since the overall trend represents the differences in
  10824. the quantile normalization step.
  10825. When running
  10826. \begin_inset Flex Glossary Term
  10827. status open
  10828. \begin_layout Plain Layout
  10829. RMA
  10830. \end_layout
  10831. \end_inset
  10832. , only the quantiles for these specific 20 arrays are used, while for
  10833. \begin_inset Flex Glossary Term
  10834. status open
  10835. \begin_layout Plain Layout
  10836. fRMA
  10837. \end_layout
  10838. \end_inset
  10839. the quantile distribution is taking from all arrays used in training.
  10840. Figure
  10841. \begin_inset CommandInset ref
  10842. LatexCommand ref
  10843. reference "fig:ma-bx-frma-frma"
  10844. plural "false"
  10845. caps "false"
  10846. noprefix "false"
  10847. \end_inset
  10848. shows a similar MA plot comparing 2 different
  10849. \begin_inset Flex Glossary Term
  10850. status open
  10851. \begin_layout Plain Layout
  10852. fRMA
  10853. \end_layout
  10854. \end_inset
  10855. normalizations, corresponding to the 6th row of Figure
  10856. \begin_inset CommandInset ref
  10857. LatexCommand ref
  10858. reference "fig:m-bx-violin"
  10859. plural "false"
  10860. caps "false"
  10861. noprefix "false"
  10862. \end_inset
  10863. .
  10864. The MA plot is very tightly centered around zero with no visible trend.
  10865. Figures
  10866. \begin_inset CommandInset ref
  10867. LatexCommand ref
  10868. reference "fig:m-pax-violin"
  10869. plural "false"
  10870. caps "false"
  10871. noprefix "false"
  10872. \end_inset
  10873. ,
  10874. \begin_inset CommandInset ref
  10875. LatexCommand ref
  10876. reference "fig:MA-PAX-rma-frma"
  10877. plural "false"
  10878. caps "false"
  10879. noprefix "false"
  10880. \end_inset
  10881. , and
  10882. \begin_inset CommandInset ref
  10883. LatexCommand ref
  10884. reference "fig:ma-bx-frma-frma"
  10885. plural "false"
  10886. caps "false"
  10887. noprefix "false"
  10888. \end_inset
  10889. show exactly the same information for the blood samples, once again comparing
  10890. the normalized expression values between normalizations for all probe sets
  10891. across 20 randomly selected test arrays.
  10892. Once again, there is a wider distribution of log ratios between RMA-normalized
  10893. values and fRMA-normalized, and a much tighter distribution when comparing
  10894. different
  10895. \begin_inset Flex Glossary Term
  10896. status open
  10897. \begin_layout Plain Layout
  10898. fRMA
  10899. \end_layout
  10900. \end_inset
  10901. normalizations to each other, indicating that the
  10902. \begin_inset Flex Glossary Term
  10903. status open
  10904. \begin_layout Plain Layout
  10905. fRMA
  10906. \end_layout
  10907. \end_inset
  10908. training process is robust to random batch sub-sampling for the blood samples
  10909. as well.
  10910. \end_layout
  10911. \begin_layout Standard
  10912. \begin_inset Float figure
  10913. wide false
  10914. sideways false
  10915. status collapsed
  10916. \begin_layout Plain Layout
  10917. \align center
  10918. \begin_inset Float figure
  10919. wide false
  10920. sideways false
  10921. status open
  10922. \begin_layout Plain Layout
  10923. \align center
  10924. \begin_inset Graphics
  10925. filename graphics/frma-pax-bx/MA-BX-RMA.fRMA-RASTER.png
  10926. lyxscale 10
  10927. width 45col%
  10928. groupId ma-frma
  10929. \end_inset
  10930. \end_layout
  10931. \begin_layout Plain Layout
  10932. \begin_inset Caption Standard
  10933. \begin_layout Plain Layout
  10934. \begin_inset CommandInset label
  10935. LatexCommand label
  10936. name "fig:ma-bx-rma-frma"
  10937. \end_inset
  10938. RMA vs.
  10939. fRMA for biopsy samples.
  10940. \end_layout
  10941. \end_inset
  10942. \end_layout
  10943. \end_inset
  10944. \begin_inset space \hfill{}
  10945. \end_inset
  10946. \begin_inset Float figure
  10947. wide false
  10948. sideways false
  10949. status collapsed
  10950. \begin_layout Plain Layout
  10951. \align center
  10952. \begin_inset Graphics
  10953. filename graphics/frma-pax-bx/MA-BX-fRMA.fRMA-RASTER.png
  10954. lyxscale 10
  10955. width 45col%
  10956. groupId ma-frma
  10957. \end_inset
  10958. \end_layout
  10959. \begin_layout Plain Layout
  10960. \begin_inset Caption Standard
  10961. \begin_layout Plain Layout
  10962. \begin_inset CommandInset label
  10963. LatexCommand label
  10964. name "fig:ma-bx-frma-frma"
  10965. \end_inset
  10966. fRMA vs fRMA for biopsy samples.
  10967. \end_layout
  10968. \end_inset
  10969. \end_layout
  10970. \end_inset
  10971. \end_layout
  10972. \begin_layout Plain Layout
  10973. \align center
  10974. \begin_inset Float figure
  10975. wide false
  10976. sideways false
  10977. status collapsed
  10978. \begin_layout Plain Layout
  10979. \align center
  10980. \begin_inset Graphics
  10981. filename graphics/frma-pax-bx/MA-PAX-RMA.fRMA-RASTER.png
  10982. lyxscale 10
  10983. width 45col%
  10984. groupId ma-frma
  10985. \end_inset
  10986. \end_layout
  10987. \begin_layout Plain Layout
  10988. \begin_inset Caption Standard
  10989. \begin_layout Plain Layout
  10990. \begin_inset CommandInset label
  10991. LatexCommand label
  10992. name "fig:MA-PAX-rma-frma"
  10993. \end_inset
  10994. RMA vs.
  10995. fRMA for blood samples.
  10996. \end_layout
  10997. \end_inset
  10998. \end_layout
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  11009. filename graphics/frma-pax-bx/MA-PAX-fRMA.fRMA-RASTER.png
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  11012. groupId ma-frma
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  11018. \begin_inset CommandInset label
  11019. LatexCommand label
  11020. name "fig:MA-PAX-frma-frma"
  11021. \end_inset
  11022. fRMA vs fRMA for blood samples.
  11023. \end_layout
  11024. \end_inset
  11025. \end_layout
  11026. \end_inset
  11027. \end_layout
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  11030. \begin_layout Plain Layout
  11031. \begin_inset Argument 1
  11032. status collapsed
  11033. \begin_layout Plain Layout
  11034. Representative MA plots comparing RMA and custom fRMA normalizations.
  11035. \end_layout
  11036. \end_inset
  11037. \begin_inset CommandInset label
  11038. LatexCommand label
  11039. name "fig:Representative-MA-plots"
  11040. \end_inset
  11041. \series bold
  11042. Representative MA plots comparing RMA and custom fRMA normalizations.
  11043. \series default
  11044. For each plot, 20 samples were normalized using 2 different normalizations,
  11045. and then averages (A) and log ratios (M) were plotted between the two different
  11046. normalizations for every probe.
  11047. For the
  11048. \begin_inset Quotes eld
  11049. \end_inset
  11050. fRMA vs fRMA
  11051. \begin_inset Quotes erd
  11052. \end_inset
  11053. plots (b & d), two different fRMA normalizations using vectors from two
  11054. independent batch samplings were compared.
  11055. Density of points is represented by blue shading, and individual outlier
  11056. points are plotted.
  11057. \end_layout
  11058. \end_inset
  11059. \end_layout
  11060. \end_inset
  11061. \end_layout
  11062. \begin_layout Subsection
  11063. SVA, voom, and array weights improve model fit for methylation array data
  11064. \end_layout
  11065. \begin_layout Standard
  11066. Figure
  11067. \begin_inset CommandInset ref
  11068. LatexCommand ref
  11069. reference "fig:meanvar-basic"
  11070. plural "false"
  11071. caps "false"
  11072. noprefix "false"
  11073. \end_inset
  11074. shows the relationship between the mean
  11075. \begin_inset Flex Glossary Term
  11076. status open
  11077. \begin_layout Plain Layout
  11078. M-value
  11079. \end_layout
  11080. \end_inset
  11081. and the standard deviation calculated for each probe in the methylation
  11082. array data set.
  11083. A few features of the data are apparent.
  11084. First, the data are very strongly bimodal, with peaks in the density around
  11085. \begin_inset Flex Glossary Term (pl)
  11086. status open
  11087. \begin_layout Plain Layout
  11088. M-value
  11089. \end_layout
  11090. \end_inset
  11091. of +4 and -4.
  11092. These modes correspond to methylation sites that are nearly 100% methylated
  11093. and nearly 100% unmethylated, respectively.
  11094. The strong bimodality indicates that a majority of probes interrogate sites
  11095. that fall into one of these two categories.
  11096. The points in between these modes represent sites that are either partially
  11097. methylated in many samples, or are fully methylated in some samples and
  11098. fully unmethylated in other samples, or some combination.
  11099. The next visible feature of the data is the W-shaped variance trend.
  11100. The upticks in the variance trend on either side are expected, based on
  11101. the sigmoid transformation exaggerating small differences at extreme
  11102. \begin_inset Flex Glossary Term (pl)
  11103. status open
  11104. \begin_layout Plain Layout
  11105. M-value
  11106. \end_layout
  11107. \end_inset
  11108. (Figure
  11109. \begin_inset CommandInset ref
  11110. LatexCommand ref
  11111. reference "fig:Sigmoid-beta-m-mapping"
  11112. plural "false"
  11113. caps "false"
  11114. noprefix "false"
  11115. \end_inset
  11116. ).
  11117. However, the uptick in the center is interesting: it indicates that sites
  11118. that are not constitutively methylated or unmethylated have a higher variance.
  11119. This could be a genuine biological effect, or it could be spurious noise
  11120. that is only observable at sites with varying methylation.
  11121. \end_layout
  11122. \begin_layout Standard
  11123. \begin_inset ERT
  11124. status open
  11125. \begin_layout Plain Layout
  11126. \backslash
  11127. afterpage{
  11128. \end_layout
  11129. \begin_layout Plain Layout
  11130. \backslash
  11131. begin{landscape}
  11132. \end_layout
  11133. \end_inset
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  11135. \begin_layout Standard
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  11137. wide false
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  11141. \begin_inset Flex TODO Note (inline)
  11142. status open
  11143. \begin_layout Plain Layout
  11144. Fix axis labels:
  11145. \begin_inset Quotes eld
  11146. \end_inset
  11147. log2 M-value
  11148. \begin_inset Quotes erd
  11149. \end_inset
  11150. is redundant because M-values are already log scale
  11151. \end_layout
  11152. \end_inset
  11153. \end_layout
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  11156. wide false
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  11162. filename graphics/methylvoom/unadj.dupcor/meanvar-trends-PAGE1-CROP-RASTER.png
  11163. lyxscale 15
  11164. width 30col%
  11165. groupId voomaw-subfig
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  11172. LatexCommand label
  11173. name "fig:meanvar-basic"
  11174. \end_inset
  11175. Mean-variance trend for analysis A.
  11176. \end_layout
  11177. \end_inset
  11178. \end_layout
  11179. \end_inset
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  11181. \end_inset
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  11189. filename graphics/methylvoom/unadj.dupcor.sva.aw/meanvar-trends-PAGE1-CROP-RASTER.png
  11190. lyxscale 15
  11191. width 30col%
  11192. groupId voomaw-subfig
  11193. \end_inset
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  11199. LatexCommand label
  11200. name "fig:meanvar-sva-aw"
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  11202. Mean-variance trend for analysis B.
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  11217. lyxscale 15
  11218. width 30col%
  11219. groupId voomaw-subfig
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  11226. LatexCommand label
  11227. name "fig:meanvar-sva-voomaw"
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  11229. Mean-variance trend after voom modeling in analysis C.
  11230. \end_layout
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  11232. \end_layout
  11233. \end_inset
  11234. \end_layout
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  11236. \begin_inset Caption Standard
  11237. \begin_layout Plain Layout
  11238. \begin_inset Argument 1
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  11240. \begin_layout Plain Layout
  11241. Mean-variance trend modeling in methylation array data.
  11242. \end_layout
  11243. \end_inset
  11244. \begin_inset CommandInset label
  11245. LatexCommand label
  11246. name "fig:-Meanvar-trend-methyl"
  11247. \end_inset
  11248. \series bold
  11249. Mean-variance trend modeling in methylation array data.
  11250. \series default
  11251. The estimated
  11252. \begin_inset Formula $\log_{2}$
  11253. \end_inset
  11254. (standard deviation) for each probe is plotted against the probe's average
  11255. M-value across all samples as a black point, with some transparency to
  11256. make over-plotting more visible, since there are about 450,000 points.
  11257. Density of points is also indicated by the dark blue contour lines.
  11258. The prior variance trend estimated by eBayes is shown in light blue, while
  11259. the lowess trend of the points is shown in red.
  11260. \end_layout
  11261. \end_inset
  11262. \end_layout
  11263. \end_inset
  11264. \end_layout
  11265. \begin_layout Standard
  11266. \begin_inset ERT
  11267. status open
  11268. \begin_layout Plain Layout
  11269. \backslash
  11270. end{landscape}
  11271. \end_layout
  11272. \begin_layout Plain Layout
  11273. }
  11274. \end_layout
  11275. \end_inset
  11276. \end_layout
  11277. \begin_layout Standard
  11278. In Figure
  11279. \begin_inset CommandInset ref
  11280. LatexCommand ref
  11281. reference "fig:meanvar-sva-aw"
  11282. plural "false"
  11283. caps "false"
  11284. noprefix "false"
  11285. \end_inset
  11286. , we see the mean-variance trend for the same methylation array data, this
  11287. time with surrogate variables and sample quality weights estimated from
  11288. the data and included in the model.
  11289. As expected, the overall average variance is smaller, since the surrogate
  11290. variables account for some of the variance.
  11291. In addition, the uptick in variance in the middle of the
  11292. \begin_inset Flex Glossary Term
  11293. status open
  11294. \begin_layout Plain Layout
  11295. M-value
  11296. \end_layout
  11297. \end_inset
  11298. range has disappeared, turning the W shape into a wide U shape.
  11299. This indicates that the excess variance in the probes with intermediate
  11300. \begin_inset Flex Glossary Term (pl)
  11301. status open
  11302. \begin_layout Plain Layout
  11303. M-value
  11304. \end_layout
  11305. \end_inset
  11306. was explained by systematic variations not correlated with known covariates,
  11307. and these variations were modeled by the surrogate variables.
  11308. The result is a nearly flat variance trend for the entire intermediate
  11309. \begin_inset Flex Glossary Term
  11310. status open
  11311. \begin_layout Plain Layout
  11312. M-value
  11313. \end_layout
  11314. \end_inset
  11315. range from about -3 to +3.
  11316. Note that this corresponds closely to the range within which the
  11317. \begin_inset Flex Glossary Term
  11318. status open
  11319. \begin_layout Plain Layout
  11320. M-value
  11321. \end_layout
  11322. \end_inset
  11323. transformation shown in Figure
  11324. \begin_inset CommandInset ref
  11325. LatexCommand ref
  11326. reference "fig:Sigmoid-beta-m-mapping"
  11327. plural "false"
  11328. caps "false"
  11329. noprefix "false"
  11330. \end_inset
  11331. is nearly linear.
  11332. In contrast, the excess variance at the extremes (greater than +3 and less
  11333. than -3) was not
  11334. \begin_inset Quotes eld
  11335. \end_inset
  11336. absorbed
  11337. \begin_inset Quotes erd
  11338. \end_inset
  11339. by the surrogate variables and remains in the plot, indicating that this
  11340. variation has no systematic component: probes with extreme
  11341. \begin_inset Flex Glossary Term (pl)
  11342. status open
  11343. \begin_layout Plain Layout
  11344. M-value
  11345. \end_layout
  11346. \end_inset
  11347. are uniformly more variable across all samples, as expected.
  11348. \end_layout
  11349. \begin_layout Standard
  11350. Figure
  11351. \begin_inset CommandInset ref
  11352. LatexCommand ref
  11353. reference "fig:meanvar-sva-voomaw"
  11354. plural "false"
  11355. caps "false"
  11356. noprefix "false"
  11357. \end_inset
  11358. shows the mean-variance trend after fitting the model with the observation
  11359. weights assigned by voom based on the mean-variance trend shown in Figure
  11360. \begin_inset CommandInset ref
  11361. LatexCommand ref
  11362. reference "fig:meanvar-sva-aw"
  11363. plural "false"
  11364. caps "false"
  11365. noprefix "false"
  11366. \end_inset
  11367. .
  11368. As expected, the weights exactly counteract the trend in the data, resulting
  11369. in a nearly flat trend centered vertically at 1 (i.e.
  11370. 0 on the log scale).
  11371. This shows that the observations with extreme
  11372. \begin_inset Flex Glossary Term (pl)
  11373. status open
  11374. \begin_layout Plain Layout
  11375. M-value
  11376. \end_layout
  11377. \end_inset
  11378. have been appropriately down-weighted to account for the fact that the
  11379. noise in those observations has been amplified by the non-linear
  11380. \begin_inset Flex Glossary Term
  11381. status open
  11382. \begin_layout Plain Layout
  11383. M-value
  11384. \end_layout
  11385. \end_inset
  11386. transformation.
  11387. In turn, this gives relatively more weight to observations in the middle
  11388. region, which are more likely to correspond to probes measuring interesting
  11389. biology (not constitutively methylated or unmethylated).
  11390. \end_layout
  11391. \begin_layout Standard
  11392. To determine whether any of the known experimental factors had an impact
  11393. on data quality, the sample quality weights estimated from the data were
  11394. tested for association with each of the experimental factors (Table
  11395. \begin_inset CommandInset ref
  11396. LatexCommand ref
  11397. reference "tab:weight-covariate-tests"
  11398. plural "false"
  11399. caps "false"
  11400. noprefix "false"
  11401. \end_inset
  11402. ).
  11403. Diabetes diagnosis was found to have a potentially significant association
  11404. with the sample weights, with a t-test p-value of
  11405. \begin_inset Formula $1.06\times10^{-3}$
  11406. \end_inset
  11407. .
  11408. Figure
  11409. \begin_inset CommandInset ref
  11410. LatexCommand ref
  11411. reference "fig:diabetes-sample-weights"
  11412. plural "false"
  11413. caps "false"
  11414. noprefix "false"
  11415. \end_inset
  11416. shows the distribution of sample weights grouped by diabetes diagnosis.
  11417. The samples from patients with
  11418. \begin_inset Flex Glossary Term
  11419. status open
  11420. \begin_layout Plain Layout
  11421. T2D
  11422. \end_layout
  11423. \end_inset
  11424. were assigned significantly lower weights than those from patients with
  11425. \begin_inset Flex Glossary Term
  11426. status open
  11427. \begin_layout Plain Layout
  11428. T1D
  11429. \end_layout
  11430. \end_inset
  11431. .
  11432. This indicates that the
  11433. \begin_inset Flex Glossary Term
  11434. status open
  11435. \begin_layout Plain Layout
  11436. T2D
  11437. \end_layout
  11438. \end_inset
  11439. samples had an overall higher variance on average across all probes.
  11440. \end_layout
  11441. \begin_layout Standard
  11442. \begin_inset Float table
  11443. wide false
  11444. sideways false
  11445. status collapsed
  11446. \begin_layout Plain Layout
  11447. \align center
  11448. \begin_inset Tabular
  11449. <lyxtabular version="3" rows="5" columns="3">
  11450. <features tabularvalignment="middle">
  11451. <column alignment="center" valignment="top">
  11452. <column alignment="center" valignment="top">
  11453. <column alignment="center" valignment="top">
  11454. <row>
  11455. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  11456. \begin_inset Text
  11457. \begin_layout Plain Layout
  11458. Covariate
  11459. \end_layout
  11460. \end_inset
  11461. </cell>
  11462. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  11463. \begin_inset Text
  11464. \begin_layout Plain Layout
  11465. Test used
  11466. \end_layout
  11467. \end_inset
  11468. </cell>
  11469. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" rightline="true" usebox="none">
  11470. \begin_inset Text
  11471. \begin_layout Plain Layout
  11472. p-value
  11473. \end_layout
  11474. \end_inset
  11475. </cell>
  11476. </row>
  11477. <row>
  11478. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  11479. \begin_inset Text
  11480. \begin_layout Plain Layout
  11481. Transplant Status
  11482. \end_layout
  11483. \end_inset
  11484. </cell>
  11485. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  11486. \begin_inset Text
  11487. \begin_layout Plain Layout
  11488. F-test
  11489. \end_layout
  11490. \end_inset
  11491. </cell>
  11492. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  11493. \begin_inset Text
  11494. \begin_layout Plain Layout
  11495. 0.404
  11496. \end_layout
  11497. \end_inset
  11498. </cell>
  11499. </row>
  11500. <row>
  11501. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  11502. \begin_inset Text
  11503. \begin_layout Plain Layout
  11504. Diabetes Diagnosis
  11505. \end_layout
  11506. \end_inset
  11507. </cell>
  11508. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  11509. \begin_inset Text
  11510. \begin_layout Plain Layout
  11511. \emph on
  11512. t
  11513. \emph default
  11514. -test
  11515. \end_layout
  11516. \end_inset
  11517. </cell>
  11518. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  11519. \begin_inset Text
  11520. \begin_layout Plain Layout
  11521. 0.00106
  11522. \end_layout
  11523. \end_inset
  11524. </cell>
  11525. </row>
  11526. <row>
  11527. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  11528. \begin_inset Text
  11529. \begin_layout Plain Layout
  11530. Sex
  11531. \end_layout
  11532. \end_inset
  11533. </cell>
  11534. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  11535. \begin_inset Text
  11536. \begin_layout Plain Layout
  11537. \emph on
  11538. t
  11539. \emph default
  11540. -test
  11541. \end_layout
  11542. \end_inset
  11543. </cell>
  11544. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  11545. \begin_inset Text
  11546. \begin_layout Plain Layout
  11547. 0.148
  11548. \end_layout
  11549. \end_inset
  11550. </cell>
  11551. </row>
  11552. <row>
  11553. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  11554. \begin_inset Text
  11555. \begin_layout Plain Layout
  11556. Age
  11557. \end_layout
  11558. \end_inset
  11559. </cell>
  11560. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  11561. \begin_inset Text
  11562. \begin_layout Plain Layout
  11563. linear regression
  11564. \end_layout
  11565. \end_inset
  11566. </cell>
  11567. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" rightline="true" usebox="none">
  11568. \begin_inset Text
  11569. \begin_layout Plain Layout
  11570. 0.212
  11571. \end_layout
  11572. \end_inset
  11573. </cell>
  11574. </row>
  11575. </lyxtabular>
  11576. \end_inset
  11577. \end_layout
  11578. \begin_layout Plain Layout
  11579. \begin_inset Caption Standard
  11580. \begin_layout Plain Layout
  11581. \begin_inset Argument 1
  11582. status collapsed
  11583. \begin_layout Plain Layout
  11584. Association of sample weights with clinical covariates in methylation array
  11585. data.
  11586. \end_layout
  11587. \end_inset
  11588. \begin_inset CommandInset label
  11589. LatexCommand label
  11590. name "tab:weight-covariate-tests"
  11591. \end_inset
  11592. \series bold
  11593. Association of sample weights with clinical covariates in methylation array
  11594. data.
  11595. \series default
  11596. Computed sample quality log weights were tested for significant association
  11597. with each of the variables in the model (1st column).
  11598. An appropriate test was selected for each variable based on whether the
  11599. variable had 2 categories (
  11600. \emph on
  11601. t
  11602. \emph default
  11603. -test), had more than 2 categories (F-test), or was numeric (linear regression).
  11604. The test selected is shown in the 2nd column.
  11605. P-values for association with the log weights are shown in the 3rd column.
  11606. No multiple testing adjustment was performed for these p-values.
  11607. \end_layout
  11608. \end_inset
  11609. \end_layout
  11610. \end_inset
  11611. \end_layout
  11612. \begin_layout Standard
  11613. \begin_inset Float figure
  11614. wide false
  11615. sideways false
  11616. status collapsed
  11617. \begin_layout Plain Layout
  11618. \begin_inset Flex TODO Note (inline)
  11619. status open
  11620. \begin_layout Plain Layout
  11621. Redo the sample weight boxplot with notches, and remove fill colors
  11622. \end_layout
  11623. \end_inset
  11624. \end_layout
  11625. \begin_layout Plain Layout
  11626. \align center
  11627. \begin_inset Graphics
  11628. filename graphics/methylvoom/unadj.dupcor.sva.voomaw/sample-weights-PAGE3-CROP.pdf
  11629. lyxscale 50
  11630. width 60col%
  11631. groupId colwidth
  11632. \end_inset
  11633. \end_layout
  11634. \begin_layout Plain Layout
  11635. \begin_inset Caption Standard
  11636. \begin_layout Plain Layout
  11637. \begin_inset Argument 1
  11638. status collapsed
  11639. \begin_layout Plain Layout
  11640. Box-and-whiskers plot of sample quality weights grouped by diabetes diagnosis.
  11641. \end_layout
  11642. \end_inset
  11643. \begin_inset CommandInset label
  11644. LatexCommand label
  11645. name "fig:diabetes-sample-weights"
  11646. \end_inset
  11647. \series bold
  11648. Box-and-whiskers plot of sample quality weights grouped by diabetes diagnosis.
  11649. \series default
  11650. Samples were grouped based on diabetes diagnosis, and the distribution of
  11651. sample quality weights for each diagnosis was plotted as a box-and-whiskers
  11652. plot
  11653. \begin_inset CommandInset citation
  11654. LatexCommand cite
  11655. key "McGill1978"
  11656. literal "false"
  11657. \end_inset
  11658. .
  11659. \end_layout
  11660. \end_inset
  11661. \end_layout
  11662. \end_inset
  11663. \end_layout
  11664. \begin_layout Standard
  11665. Table
  11666. \begin_inset CommandInset ref
  11667. LatexCommand ref
  11668. reference "tab:methyl-num-signif"
  11669. plural "false"
  11670. caps "false"
  11671. noprefix "false"
  11672. \end_inset
  11673. shows the number of significantly differentially methylated probes reported
  11674. by each analysis for each comparison of interest at an
  11675. \begin_inset Flex Glossary Term
  11676. status open
  11677. \begin_layout Plain Layout
  11678. FDR
  11679. \end_layout
  11680. \end_inset
  11681. of 10%.
  11682. As expected, the more elaborate analyses, B and C, report more significant
  11683. probes than the more basic analysis A, consistent with the conclusions
  11684. above that the data contain hidden systematic variations that must be modeled.
  11685. Table
  11686. \begin_inset CommandInset ref
  11687. LatexCommand ref
  11688. reference "tab:methyl-est-nonnull"
  11689. plural "false"
  11690. caps "false"
  11691. noprefix "false"
  11692. \end_inset
  11693. shows the estimated number differentially methylated probes for each test
  11694. from each analysis.
  11695. This was computed by estimating the proportion of null hypotheses that
  11696. were true using the method of
  11697. \begin_inset CommandInset citation
  11698. LatexCommand cite
  11699. key "Phipson2013Thesis"
  11700. literal "false"
  11701. \end_inset
  11702. and subtracting that fraction from the total number of probes, yielding
  11703. an estimate of the number of null hypotheses that are false based on the
  11704. distribution of p-values across the entire dataset.
  11705. Note that this does not identify which null hypotheses should be rejected
  11706. (i.e.
  11707. which probes are significant); it only estimates the true number of such
  11708. probes.
  11709. Once again, analyses B and C result it much larger estimates for the number
  11710. of differentially methylated probes.
  11711. In this case, analysis C, the only analysis that includes voom, estimates
  11712. the largest number of differentially methylated probes for all 3 contrasts.
  11713. If the assumptions of all the methods employed hold, then this represents
  11714. a gain in statistical power over the simpler analysis A.
  11715. Figure
  11716. \begin_inset CommandInset ref
  11717. LatexCommand ref
  11718. reference "fig:meth-p-value-histograms"
  11719. plural "false"
  11720. caps "false"
  11721. noprefix "false"
  11722. \end_inset
  11723. shows the p-value distributions for each test, from which the numbers in
  11724. Table
  11725. \begin_inset CommandInset ref
  11726. LatexCommand ref
  11727. reference "tab:methyl-est-nonnull"
  11728. plural "false"
  11729. caps "false"
  11730. noprefix "false"
  11731. \end_inset
  11732. were generated.
  11733. The distributions for analysis A all have a dip in density near zero, which
  11734. is a strong sign of a poor model fit.
  11735. The histograms for analyses B and C are more well-behaved, with a uniform
  11736. component stretching all the way from 0 to 1 representing the probes for
  11737. which the null hypotheses is true (no differential methylation), and a
  11738. zero-biased component representing the probes for which the null hypothesis
  11739. is false (differentially methylated).
  11740. These histograms do not indicate any major issues with the model fit.
  11741. \end_layout
  11742. \begin_layout Standard
  11743. \begin_inset Float table
  11744. wide false
  11745. sideways false
  11746. status collapsed
  11747. \begin_layout Plain Layout
  11748. \align center
  11749. \begin_inset Flex TODO Note (inline)
  11750. status open
  11751. \begin_layout Plain Layout
  11752. Consider transposing these tables
  11753. \end_layout
  11754. \end_inset
  11755. \end_layout
  11756. \begin_layout Plain Layout
  11757. \begin_inset Float table
  11758. wide false
  11759. sideways false
  11760. status open
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  11778. \begin_inset Text
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  11782. \end_inset
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  11801. Contrast
  11802. \end_layout
  11803. \end_inset
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  11806. \begin_inset Text
  11807. \begin_layout Plain Layout
  11808. A
  11809. \end_layout
  11810. \end_inset
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  11813. \begin_inset Text
  11814. \begin_layout Plain Layout
  11815. B
  11816. \end_layout
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  11820. \begin_inset Text
  11821. \begin_layout Plain Layout
  11822. C
  11823. \end_layout
  11824. \end_inset
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  11828. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  11829. \begin_inset Text
  11830. \begin_layout Plain Layout
  11831. TX vs AR
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  11859. \begin_inset Text
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  11861. TX vs ADNR
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  11889. \begin_inset Text
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  11892. \end_layout
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  11922. \begin_layout Plain Layout
  11923. \begin_inset CommandInset label
  11924. LatexCommand label
  11925. name "tab:methyl-num-signif"
  11926. \end_inset
  11927. Number of probes significant at 10% FDR.
  11928. \end_layout
  11929. \end_inset
  11930. \end_layout
  11931. \end_inset
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  11944. <column alignment="center" valignment="top">
  11945. <column alignment="center" valignment="top">
  11946. <column alignment="center" valignment="top">
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  11976. \begin_inset Text
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  11978. Contrast
  11979. \end_layout
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  11984. \begin_layout Plain Layout
  11985. A
  11986. \end_layout
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  11990. \begin_inset Text
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  11993. \end_layout
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  11997. \begin_inset Text
  11998. \begin_layout Plain Layout
  11999. C
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  12004. <row>
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  12006. \begin_inset Text
  12007. \begin_layout Plain Layout
  12008. TX vs AR
  12009. \end_layout
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  12028. \begin_layout Plain Layout
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  12030. \end_layout
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  12034. <row>
  12035. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  12036. \begin_inset Text
  12037. \begin_layout Plain Layout
  12038. TX vs ADNR
  12039. \end_layout
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  12043. \begin_inset Text
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  12058. \begin_layout Plain Layout
  12059. 13,086
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  12066. \begin_inset Text
  12067. \begin_layout Plain Layout
  12068. TX vs CAN
  12069. \end_layout
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  12100. \begin_inset CommandInset label
  12101. LatexCommand label
  12102. name "tab:methyl-est-nonnull"
  12103. \end_inset
  12104. Estimated number of non-null tests, using the method of averaging local
  12105. FDR values
  12106. \begin_inset CommandInset citation
  12107. LatexCommand cite
  12108. key "Phipson2013Thesis"
  12109. literal "false"
  12110. \end_inset
  12111. .
  12112. \end_layout
  12113. \end_inset
  12114. \end_layout
  12115. \end_inset
  12116. \end_layout
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  12118. \begin_inset Caption Standard
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  12120. \begin_inset Argument 1
  12121. status collapsed
  12122. \begin_layout Plain Layout
  12123. Estimates of degree of differential methylation in for each contrast in
  12124. each analysis.
  12125. \end_layout
  12126. \end_inset
  12127. \series bold
  12128. Estimates of degree of differential methylation in for each contrast in
  12129. each analysis.
  12130. \series default
  12131. For each of the analyses in Table
  12132. \begin_inset CommandInset ref
  12133. LatexCommand ref
  12134. reference "tab:Summary-of-meth-analysis"
  12135. plural "false"
  12136. caps "false"
  12137. noprefix "false"
  12138. \end_inset
  12139. , these tables show the number of probes called significantly differentially
  12140. methylated at a threshold of 10% FDR for each comparison between TX and
  12141. the other 3 transplant statuses (a) and the estimated total number of probes
  12142. that are differentially methylated (b).
  12143. \end_layout
  12144. \end_inset
  12145. \end_layout
  12146. \end_inset
  12147. \end_layout
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  12170. \series bold
  12171. \begin_inset Caption Standard
  12172. \begin_layout Plain Layout
  12173. AR vs.
  12174. TX, Analysis A
  12175. \end_layout
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  12195. \series bold
  12196. \begin_inset Caption Standard
  12197. \begin_layout Plain Layout
  12198. ADNR vs.
  12199. TX, Analysis A
  12200. \end_layout
  12201. \end_inset
  12202. \end_layout
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  12220. \series bold
  12221. \begin_inset Caption Standard
  12222. \begin_layout Plain Layout
  12223. CAN vs.
  12224. TX, Analysis A
  12225. \end_layout
  12226. \end_inset
  12227. \end_layout
  12228. \end_inset
  12229. \end_layout
  12230. \begin_layout Plain Layout
  12231. \align center
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  12247. \series bold
  12248. \begin_inset Caption Standard
  12249. \begin_layout Plain Layout
  12250. AR vs.
  12251. TX, Analysis B
  12252. \end_layout
  12253. \end_inset
  12254. \end_layout
  12255. \end_inset
  12256. \begin_inset space \hfill{}
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  12275. ADNR vs.
  12276. TX, Analysis B
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  12287. \begin_layout Plain Layout
  12288. \align center
  12289. \begin_inset Graphics
  12290. filename graphics/methylvoom/unadj.dupcor.sva.aw/pval-histograms-PAGE3.pdf
  12291. lyxscale 33
  12292. width 30col%
  12293. groupId meth-pval-hist
  12294. \end_inset
  12295. \end_layout
  12296. \begin_layout Plain Layout
  12297. \series bold
  12298. \begin_inset Caption Standard
  12299. \begin_layout Plain Layout
  12300. CAN vs.
  12301. TX, Analysis B
  12302. \end_layout
  12303. \end_inset
  12304. \end_layout
  12305. \end_inset
  12306. \end_layout
  12307. \begin_layout Plain Layout
  12308. \align center
  12309. \series bold
  12310. \begin_inset Float figure
  12311. wide false
  12312. sideways false
  12313. status collapsed
  12314. \begin_layout Plain Layout
  12315. \align center
  12316. \begin_inset Graphics
  12317. filename graphics/methylvoom/unadj.dupcor.sva.voomaw/pval-histograms-PAGE1.pdf
  12318. lyxscale 33
  12319. width 30col%
  12320. groupId meth-pval-hist
  12321. \end_inset
  12322. \end_layout
  12323. \begin_layout Plain Layout
  12324. \series bold
  12325. \begin_inset Caption Standard
  12326. \begin_layout Plain Layout
  12327. AR vs.
  12328. TX, Analysis C
  12329. \end_layout
  12330. \end_inset
  12331. \end_layout
  12332. \end_inset
  12333. \begin_inset space \hfill{}
  12334. \end_inset
  12335. \begin_inset Float figure
  12336. wide false
  12337. sideways false
  12338. status collapsed
  12339. \begin_layout Plain Layout
  12340. \align center
  12341. \begin_inset Graphics
  12342. filename graphics/methylvoom/unadj.dupcor.sva.voomaw/pval-histograms-PAGE2.pdf
  12343. lyxscale 33
  12344. width 30col%
  12345. groupId meth-pval-hist
  12346. \end_inset
  12347. \end_layout
  12348. \begin_layout Plain Layout
  12349. \series bold
  12350. \begin_inset Caption Standard
  12351. \begin_layout Plain Layout
  12352. ADNR vs.
  12353. TX, Analysis C
  12354. \end_layout
  12355. \end_inset
  12356. \end_layout
  12357. \end_inset
  12358. \begin_inset space \hfill{}
  12359. \end_inset
  12360. \begin_inset Float figure
  12361. wide false
  12362. sideways false
  12363. status collapsed
  12364. \begin_layout Plain Layout
  12365. \align center
  12366. \begin_inset Graphics
  12367. filename graphics/methylvoom/unadj.dupcor.sva.voomaw/pval-histograms-PAGE3.pdf
  12368. lyxscale 33
  12369. width 30col%
  12370. groupId meth-pval-hist
  12371. \end_inset
  12372. \end_layout
  12373. \begin_layout Plain Layout
  12374. \series bold
  12375. \begin_inset Caption Standard
  12376. \begin_layout Plain Layout
  12377. CAN vs.
  12378. TX, Analysis C
  12379. \end_layout
  12380. \end_inset
  12381. \end_layout
  12382. \end_inset
  12383. \end_layout
  12384. \begin_layout Plain Layout
  12385. \begin_inset Caption Standard
  12386. \begin_layout Plain Layout
  12387. \begin_inset Argument 1
  12388. status collapsed
  12389. \begin_layout Plain Layout
  12390. Probe p-value histograms for each contrast in each analysis.
  12391. \end_layout
  12392. \end_inset
  12393. \begin_inset CommandInset label
  12394. LatexCommand label
  12395. name "fig:meth-p-value-histograms"
  12396. \end_inset
  12397. \series bold
  12398. Probe p-value histograms for each contrast in each analysis.
  12399. \series default
  12400. For each differential methylation test of interest, the distribution of
  12401. p-values across all probes is plotted as a histogram.
  12402. The red solid line indicates the density that would be expected under the
  12403. null hypothesis for all probes (a
  12404. \begin_inset Formula $\mathrm{Uniform}(0,1)$
  12405. \end_inset
  12406. distribution), while the blue dotted line indicates the fraction of p-values
  12407. that actually follow the null hypothesis (
  12408. \begin_inset Formula $\hat{\pi}_{0}$
  12409. \end_inset
  12410. ) estimated using the method of averaging local FDR values
  12411. \begin_inset CommandInset citation
  12412. LatexCommand cite
  12413. key "Phipson2013Thesis"
  12414. literal "false"
  12415. \end_inset
  12416. .
  12417. A blue line is only shown in each plot if the estimate of
  12418. \begin_inset Formula $\hat{\pi}_{0}$
  12419. \end_inset
  12420. for that p-value distribution is smaller than 1.
  12421. \end_layout
  12422. \end_inset
  12423. \end_layout
  12424. \end_inset
  12425. \end_layout
  12426. \begin_layout Standard
  12427. \begin_inset Flex TODO Note (inline)
  12428. status open
  12429. \begin_layout Plain Layout
  12430. If time allows, maybe generate the PCA plots before/after SVA effect subtraction
  12431. ?
  12432. \end_layout
  12433. \end_inset
  12434. \end_layout
  12435. \begin_layout Section
  12436. Discussion
  12437. \end_layout
  12438. \begin_layout Subsection
  12439. fRMA achieves clinically applicable normalization without sacrificing classifica
  12440. tion performance
  12441. \end_layout
  12442. \begin_layout Standard
  12443. As shown in Figure
  12444. \begin_inset CommandInset ref
  12445. LatexCommand ref
  12446. reference "fig:Classifier-probabilities-RMA"
  12447. plural "false"
  12448. caps "false"
  12449. noprefix "false"
  12450. \end_inset
  12451. , improper normalization, particularly separate normalization of training
  12452. and test samples, leads to unwanted biases in classification.
  12453. In a controlled experimental context, it is always possible to correct
  12454. this issue by normalizing all experimental samples together.
  12455. However, because it is not feasible to normalize all samples together in
  12456. a clinical context, a single-channel normalization is required.
  12457. \end_layout
  12458. \begin_layout Standard
  12459. The major concern in using a single-channel normalization is that non-single-cha
  12460. nnel methods can share information between arrays to improve the normalization,
  12461. and single-channel methods risk sacrificing the gains in normalization
  12462. accuracy that come from this information sharing.
  12463. In the case of
  12464. \begin_inset Flex Glossary Term
  12465. status open
  12466. \begin_layout Plain Layout
  12467. RMA
  12468. \end_layout
  12469. \end_inset
  12470. , this information sharing is accomplished through quantile normalization
  12471. and median polish steps.
  12472. The need for information sharing in quantile normalization can easily be
  12473. removed by learning a fixed set of quantiles from external data and normalizing
  12474. each array to these fixed quantiles, instead of the quantiles of the data
  12475. itself.
  12476. As long as the fixed quantiles are reasonable, the result will be similar
  12477. to standard
  12478. \begin_inset Flex Glossary Term
  12479. status open
  12480. \begin_layout Plain Layout
  12481. RMA
  12482. \end_layout
  12483. \end_inset
  12484. .
  12485. However, there is no analogous way to eliminate cross-array information
  12486. sharing in the median polish step, so
  12487. \begin_inset Flex Glossary Term
  12488. status open
  12489. \begin_layout Plain Layout
  12490. fRMA
  12491. \end_layout
  12492. \end_inset
  12493. replaces this with a weighted average of probes on each array, with the
  12494. weights learned from external data.
  12495. This step of
  12496. \begin_inset Flex Glossary Term
  12497. status open
  12498. \begin_layout Plain Layout
  12499. fRMA
  12500. \end_layout
  12501. \end_inset
  12502. has the greatest potential to diverge from RMA in undesirable ways.
  12503. \end_layout
  12504. \begin_layout Standard
  12505. However, when run on real data,
  12506. \begin_inset Flex Glossary Term
  12507. status open
  12508. \begin_layout Plain Layout
  12509. fRMA
  12510. \end_layout
  12511. \end_inset
  12512. performed at least as well as
  12513. \begin_inset Flex Glossary Term
  12514. status open
  12515. \begin_layout Plain Layout
  12516. RMA
  12517. \end_layout
  12518. \end_inset
  12519. in both the internal validation and external validation tests.
  12520. This shows that
  12521. \begin_inset Flex Glossary Term
  12522. status open
  12523. \begin_layout Plain Layout
  12524. fRMA
  12525. \end_layout
  12526. \end_inset
  12527. can be used to normalize individual clinical samples in a class prediction
  12528. context without sacrificing the classifier performance that would be obtained
  12529. by using the more well-established
  12530. \begin_inset Flex Glossary Term
  12531. status open
  12532. \begin_layout Plain Layout
  12533. RMA
  12534. \end_layout
  12535. \end_inset
  12536. for normalization.
  12537. The other single-channel normalization method considered,
  12538. \begin_inset Flex Glossary Term
  12539. status open
  12540. \begin_layout Plain Layout
  12541. SCAN
  12542. \end_layout
  12543. \end_inset
  12544. , showed some loss of
  12545. \begin_inset Flex Glossary Term
  12546. status open
  12547. \begin_layout Plain Layout
  12548. AUC
  12549. \end_layout
  12550. \end_inset
  12551. in the external validation test.
  12552. Based on these results,
  12553. \begin_inset Flex Glossary Term
  12554. status open
  12555. \begin_layout Plain Layout
  12556. fRMA
  12557. \end_layout
  12558. \end_inset
  12559. is the preferred normalization for clinical samples in a class prediction
  12560. context.
  12561. \end_layout
  12562. \begin_layout Subsection
  12563. Robust fRMA vectors can be generated for new array platforms
  12564. \end_layout
  12565. \begin_layout Standard
  12566. \begin_inset Flex TODO Note (inline)
  12567. status open
  12568. \begin_layout Plain Layout
  12569. Look up the exact numbers, do a find & replace for
  12570. \begin_inset Quotes eld
  12571. \end_inset
  12572. 850
  12573. \begin_inset Quotes erd
  12574. \end_inset
  12575. \end_layout
  12576. \end_inset
  12577. \end_layout
  12578. \begin_layout Standard
  12579. The published
  12580. \begin_inset Flex Glossary Term
  12581. status open
  12582. \begin_layout Plain Layout
  12583. fRMA
  12584. \end_layout
  12585. \end_inset
  12586. normalization vectors for the hgu133plus2 platform were generated from
  12587. a set of about 850 samples chosen from a wide range of tissues, which the
  12588. authors determined was sufficient to generate a robust set of normalization
  12589. vectors that could be applied across all tissues
  12590. \begin_inset CommandInset citation
  12591. LatexCommand cite
  12592. key "McCall2010"
  12593. literal "false"
  12594. \end_inset
  12595. .
  12596. Since we only had hthgu133pluspm for 2 tissues of interest, our needs were
  12597. more modest.
  12598. Even using only 130 samples in 26 batches of 5 samples each for kidney
  12599. biopsies, we were able to train a robust set of
  12600. \begin_inset Flex Glossary Term
  12601. status open
  12602. \begin_layout Plain Layout
  12603. fRMA
  12604. \end_layout
  12605. \end_inset
  12606. normalization vectors that were not meaningfully affected by the random
  12607. selection of 5 samples from each batch.
  12608. As expected, the training process was just as robust for the blood samples
  12609. with 230 samples in 46 batches of 5 samples each.
  12610. Because these vectors were each generated using training samples from a
  12611. single tissue, they are not suitable for general use, unlike the vectors
  12612. provided with
  12613. \begin_inset Flex Glossary Term
  12614. status open
  12615. \begin_layout Plain Layout
  12616. fRMA
  12617. \end_layout
  12618. \end_inset
  12619. itself.
  12620. They are purpose-built for normalizing a specific type of sample on a specific
  12621. platform.
  12622. This is a mostly acceptable limitation in the context of developing a machine
  12623. learning classifier for diagnosing a disease based on samples of a specific
  12624. tissue.
  12625. \end_layout
  12626. \begin_layout Standard
  12627. \begin_inset Flex TODO Note (inline)
  12628. status open
  12629. \begin_layout Plain Layout
  12630. Talk about how these vectors can be used for any data from these tissues
  12631. on this platform even though they were custom made for this data set.
  12632. \end_layout
  12633. \end_inset
  12634. \end_layout
  12635. \begin_layout Standard
  12636. \begin_inset Flex TODO Note (inline)
  12637. status open
  12638. \begin_layout Plain Layout
  12639. How to bring up that these custom vectors were used in another project by
  12640. someone else that was never published?
  12641. \end_layout
  12642. \end_inset
  12643. \end_layout
  12644. \begin_layout Subsection
  12645. Methylation array data can be successfully analyzed using existing techniques,
  12646. but machine learning poses additional challenges
  12647. \end_layout
  12648. \begin_layout Standard
  12649. Both analysis strategies B and C both yield a reasonable analysis, with
  12650. a mean-variance trend that matches the expected behavior for the non-linear
  12651. \begin_inset Flex Glossary Term
  12652. status open
  12653. \begin_layout Plain Layout
  12654. M-value
  12655. \end_layout
  12656. \end_inset
  12657. transformation (Figure
  12658. \begin_inset CommandInset ref
  12659. LatexCommand ref
  12660. reference "fig:meanvar-sva-aw"
  12661. plural "false"
  12662. caps "false"
  12663. noprefix "false"
  12664. \end_inset
  12665. ) and well-behaved p-value distributions (Figure
  12666. \begin_inset CommandInset ref
  12667. LatexCommand ref
  12668. reference "fig:meth-p-value-histograms"
  12669. plural "false"
  12670. caps "false"
  12671. noprefix "false"
  12672. \end_inset
  12673. ).
  12674. These two analyses also yield similar numbers of significant probes (Table
  12675. \begin_inset CommandInset ref
  12676. LatexCommand ref
  12677. reference "tab:methyl-num-signif"
  12678. plural "false"
  12679. caps "false"
  12680. noprefix "false"
  12681. \end_inset
  12682. ) and similar estimates of the number of differentially methylated probes
  12683. (Table
  12684. \begin_inset CommandInset ref
  12685. LatexCommand ref
  12686. reference "tab:methyl-est-nonnull"
  12687. plural "false"
  12688. caps "false"
  12689. noprefix "false"
  12690. \end_inset
  12691. ).
  12692. The main difference between these two analyses is the method used to account
  12693. for the mean-variance trend.
  12694. In analysis B, the trend is estimated and applied at the probe level: each
  12695. probe's estimated variance is squeezed toward the trend using an empirical
  12696. Bayes procedure (Figure
  12697. \begin_inset CommandInset ref
  12698. LatexCommand ref
  12699. reference "fig:meanvar-sva-aw"
  12700. plural "false"
  12701. caps "false"
  12702. noprefix "false"
  12703. \end_inset
  12704. ).
  12705. In analysis C, the trend is still estimated at the probe level, but instead
  12706. of estimating a single variance value shared across all observations for
  12707. a given probe, the voom method computes an initial estimate of the variance
  12708. for each observation individually based on where its model-fitted
  12709. \begin_inset Flex Glossary Term
  12710. status open
  12711. \begin_layout Plain Layout
  12712. M-value
  12713. \end_layout
  12714. \end_inset
  12715. falls on the trend line and then assigns inverse-variance weights to model
  12716. the difference in variance between observations.
  12717. An overall variance is still estimated for each probe using the same empirical
  12718. Bayes method, but now the residual trend is flat (Figure
  12719. \begin_inset CommandInset ref
  12720. LatexCommand ref
  12721. reference "fig:meanvar-sva-voomaw"
  12722. plural "false"
  12723. caps "false"
  12724. noprefix "false"
  12725. \end_inset
  12726. ), indicating that the mean-variance trend is adequately modeled by scaling
  12727. the estimated variance for each observation using the weights computed
  12728. by voom.
  12729. \end_layout
  12730. \begin_layout Standard
  12731. The difference between the standard empirical Bayes trended variance modeling
  12732. (analysis B) and voom (analysis C) is analogous to the difference between
  12733. a t-test with equal variance and a t-test with unequal variance, except
  12734. that the unequal group variances used in the latter test are estimated
  12735. based on the mean-variance trend from all the probes rather than the data
  12736. for the specific probe being tested, thus stabilizing the group variance
  12737. estimates by sharing information between probes.
  12738. Allowing voom to model the variance using observation weights in this manner
  12739. allows the linear model fit to concentrate statistical power where it will
  12740. do the most good.
  12741. For example, if a particular probe's
  12742. \begin_inset Flex Glossary Term (pl)
  12743. status open
  12744. \begin_layout Plain Layout
  12745. M-value
  12746. \end_layout
  12747. \end_inset
  12748. are always at the extreme of the
  12749. \begin_inset Flex Glossary Term
  12750. status open
  12751. \begin_layout Plain Layout
  12752. M-value
  12753. \end_layout
  12754. \end_inset
  12755. range (e.g.
  12756. less than -4) for
  12757. \begin_inset Flex Glossary Term
  12758. status open
  12759. \begin_layout Plain Layout
  12760. ADNR
  12761. \end_layout
  12762. \end_inset
  12763. samples, but the
  12764. \begin_inset Flex Glossary Term (pl)
  12765. status open
  12766. \begin_layout Plain Layout
  12767. M-value
  12768. \end_layout
  12769. \end_inset
  12770. for that probe in
  12771. \begin_inset Flex Glossary Term
  12772. status open
  12773. \begin_layout Plain Layout
  12774. TX
  12775. \end_layout
  12776. \end_inset
  12777. and
  12778. \begin_inset Flex Glossary Term
  12779. status open
  12780. \begin_layout Plain Layout
  12781. CAN
  12782. \end_layout
  12783. \end_inset
  12784. samples are within the flat region of the mean-variance trend (between
  12785. \begin_inset Formula $-3$
  12786. \end_inset
  12787. and
  12788. \begin_inset Formula $+3$
  12789. \end_inset
  12790. ), voom is able to down-weight the contribution of the high-variance
  12791. \begin_inset Flex Glossary Term (pl)
  12792. status open
  12793. \begin_layout Plain Layout
  12794. M-value
  12795. \end_layout
  12796. \end_inset
  12797. from the
  12798. \begin_inset Flex Glossary Term
  12799. status open
  12800. \begin_layout Plain Layout
  12801. ADNR
  12802. \end_layout
  12803. \end_inset
  12804. samples in order to gain more statistical power while testing for differential
  12805. methylation between
  12806. \begin_inset Flex Glossary Term
  12807. status open
  12808. \begin_layout Plain Layout
  12809. TX
  12810. \end_layout
  12811. \end_inset
  12812. and
  12813. \begin_inset Flex Glossary Term
  12814. status open
  12815. \begin_layout Plain Layout
  12816. CAN
  12817. \end_layout
  12818. \end_inset
  12819. .
  12820. In contrast, modeling the mean-variance trend only at the probe level would
  12821. combine the high-variance
  12822. \begin_inset Flex Glossary Term
  12823. status open
  12824. \begin_layout Plain Layout
  12825. ADNR
  12826. \end_layout
  12827. \end_inset
  12828. samples and lower-variance samples from other conditions and estimate an
  12829. intermediate variance for this probe.
  12830. In practice, analysis B shows that this approach is adequate, but the voom
  12831. approach in analysis C performs at least as well on all model fit criteria
  12832. and yields a larger estimate for the number of differentially methylated
  12833. genes,
  12834. \emph on
  12835. and
  12836. \emph default
  12837. it matches up slightly better with the theoretical properties of the data.
  12838. \end_layout
  12839. \begin_layout Standard
  12840. The significant association of diabetes diagnosis with sample quality is
  12841. interesting.
  12842. The samples with
  12843. \begin_inset Flex Glossary Term
  12844. status open
  12845. \begin_layout Plain Layout
  12846. T2D
  12847. \end_layout
  12848. \end_inset
  12849. tended to have more variation, averaged across all probes, than those with
  12850. \begin_inset Flex Glossary Term
  12851. status open
  12852. \begin_layout Plain Layout
  12853. T1D
  12854. \end_layout
  12855. \end_inset
  12856. .
  12857. This is consistent with the consensus that
  12858. \begin_inset Flex Glossary Term
  12859. status open
  12860. \begin_layout Plain Layout
  12861. T2D
  12862. \end_layout
  12863. \end_inset
  12864. and the associated metabolic syndrome represent a broad dysregulation of
  12865. the body's endocrine signaling related to metabolism
  12866. \begin_inset CommandInset citation
  12867. LatexCommand cite
  12868. key "Volkmar2012,Hall2018,Yokoi2018"
  12869. literal "false"
  12870. \end_inset
  12871. .
  12872. This dysregulation could easily manifest as a greater degree of variation
  12873. in the DNA methylation patterns of affected tissues.
  12874. In contrast,
  12875. \begin_inset Flex Glossary Term
  12876. status open
  12877. \begin_layout Plain Layout
  12878. T1D
  12879. \end_layout
  12880. \end_inset
  12881. has a more specific cause and effect, so a less variable methylation signature
  12882. is expected.
  12883. \end_layout
  12884. \begin_layout Standard
  12885. This preliminary analysis suggests that some degree of differential methylation
  12886. exists between
  12887. \begin_inset Flex Glossary Term
  12888. status open
  12889. \begin_layout Plain Layout
  12890. TX
  12891. \end_layout
  12892. \end_inset
  12893. and each of the three types of transplant disfunction studied.
  12894. Hence, it may be feasible to train a classifier to diagnose transplant
  12895. disfunction from DNA methylation array data.
  12896. However, the major importance of both
  12897. \begin_inset Flex Glossary Term
  12898. status open
  12899. \begin_layout Plain Layout
  12900. SVA
  12901. \end_layout
  12902. \end_inset
  12903. and sample quality weighting for proper modeling of this data poses significant
  12904. challenges for any attempt at a machine learning on data of similar quality.
  12905. While these are easily used in a modeling context with full sample information,
  12906. neither of these methods is directly applicable in a machine learning context,
  12907. where the diagnosis is not known ahead of time.
  12908. If a machine learning approach for methylation-based diagnosis is to be
  12909. pursued, it will either require machine-learning-friendly methods to address
  12910. the same systematic trends in the data that
  12911. \begin_inset Flex Glossary Term
  12912. status open
  12913. \begin_layout Plain Layout
  12914. SVA
  12915. \end_layout
  12916. \end_inset
  12917. and sample quality weighting address, or it will require higher quality
  12918. data with substantially less systematic perturbation of the data.
  12919. \end_layout
  12920. \begin_layout Section
  12921. Future Directions
  12922. \end_layout
  12923. \begin_layout Standard
  12924. \begin_inset Flex TODO Note (inline)
  12925. status open
  12926. \begin_layout Plain Layout
  12927. Some work was already being done with the existing fRMA vectors.
  12928. Do I mention that here?
  12929. \end_layout
  12930. \end_inset
  12931. \end_layout
  12932. \begin_layout Subsection
  12933. Improving fRMA to allow training from batches of unequal size
  12934. \end_layout
  12935. \begin_layout Standard
  12936. Because the tools for building
  12937. \begin_inset Flex Glossary Term
  12938. status open
  12939. \begin_layout Plain Layout
  12940. fRMA
  12941. \end_layout
  12942. \end_inset
  12943. normalization vectors require equal-size batches, many samples must be
  12944. discarded from the training data.
  12945. This is undesirable for a few reasons.
  12946. First, more data is simply better, all other things being equal.
  12947. In this case,
  12948. \begin_inset Quotes eld
  12949. \end_inset
  12950. better
  12951. \begin_inset Quotes erd
  12952. \end_inset
  12953. means a more precise estimate of normalization parameters.
  12954. In addition, the samples to be discarded must be chosen arbitrarily, which
  12955. introduces an unnecessary element of randomness into the estimation process.
  12956. While the randomness can be made deterministic by setting a consistent
  12957. random seed, the need for equal size batches also introduces a need for
  12958. the analyst to decide on the appropriate trade-off between batch size and
  12959. the number of batches.
  12960. This introduces an unnecessary and undesirable
  12961. \begin_inset Quotes eld
  12962. \end_inset
  12963. researcher degree of freedom
  12964. \begin_inset Quotes erd
  12965. \end_inset
  12966. into the analysis, since the generated normalization vectors now depend
  12967. on the choice of batch size based on vague selection criteria and instinct,
  12968. which can unintentionally introduce bias if the researcher chooses a batch
  12969. size based on what seems to yield the most favorable downstream results
  12970. \begin_inset CommandInset citation
  12971. LatexCommand cite
  12972. key "Simmons2011"
  12973. literal "false"
  12974. \end_inset
  12975. .
  12976. \end_layout
  12977. \begin_layout Standard
  12978. Fortunately, the requirement for equal-size batches is not inherent to the
  12979. \begin_inset Flex Glossary Term
  12980. status open
  12981. \begin_layout Plain Layout
  12982. fRMA
  12983. \end_layout
  12984. \end_inset
  12985. algorithm but rather a limitation of the implementation in the
  12986. \begin_inset Flex Code
  12987. status open
  12988. \begin_layout Plain Layout
  12989. frmaTools
  12990. \end_layout
  12991. \end_inset
  12992. package.
  12993. In personal communication, the package's author, Matthew McCall, has indicated
  12994. that with some work, it should be possible to improve the implementation
  12995. to work with batches of unequal sizes.
  12996. The current implementation ignores the batch size when calculating with-batch
  12997. and between-batch residual variances, since the batch size constant cancels
  12998. out later in the calculations as long as all batches are of equal size.
  12999. Hence, the calculations of these parameters would need to be modified to
  13000. remove this optimization and properly calculate the variances using the
  13001. full formula.
  13002. Once this modification is made, a new strategy would need to be developed
  13003. for assessing the stability of parameter estimates, since the random sub-sampli
  13004. ng step is eliminated, meaning that different sub-samplings can no longer
  13005. be compared as in Figures
  13006. \begin_inset CommandInset ref
  13007. LatexCommand ref
  13008. reference "fig:frma-violin"
  13009. plural "false"
  13010. caps "false"
  13011. noprefix "false"
  13012. \end_inset
  13013. and
  13014. \begin_inset CommandInset ref
  13015. LatexCommand ref
  13016. reference "fig:Representative-MA-plots"
  13017. plural "false"
  13018. caps "false"
  13019. noprefix "false"
  13020. \end_inset
  13021. .
  13022. Bootstrap resampling is likely a good candidate here: sample many training
  13023. sets of equal size from the existing training set with replacement, estimate
  13024. parameters from each resampled training set, and compare the estimated
  13025. parameters between bootstraps in order to quantify the variability in each
  13026. parameter's estimation.
  13027. \end_layout
  13028. \begin_layout Subsection
  13029. Developing methylation arrays as a diagnostic tool for kidney transplant
  13030. rejection
  13031. \end_layout
  13032. \begin_layout Standard
  13033. The current study has showed that DNA methylation, as assayed by Illumina
  13034. 450k methylation arrays, has some potential for diagnosing transplant dysfuncti
  13035. ons, including rejection.
  13036. However, very few probes could be confidently identified as differentially
  13037. methylated between healthy and dysfunctional transplants.
  13038. One likely explanation for this is the predominant influence of unobserved
  13039. confounding factors.
  13040. \begin_inset Flex Glossary Term
  13041. status open
  13042. \begin_layout Plain Layout
  13043. SVA
  13044. \end_layout
  13045. \end_inset
  13046. can model and correct for such factors, but the correction can never be
  13047. perfect, so some degree of unwanted systematic variation will always remain
  13048. after
  13049. \begin_inset Flex Glossary Term
  13050. status open
  13051. \begin_layout Plain Layout
  13052. SVA
  13053. \end_layout
  13054. \end_inset
  13055. correction.
  13056. If the effect size of the confounding factors was similar to that of the
  13057. factor of interest (in this case, transplant status), this would be an
  13058. acceptable limitation, since removing most of the confounding factors'
  13059. effects would allow the main effect to stand out.
  13060. However, in this data set, the confounding factors have a much larger effect
  13061. size than transplant status, which means that the small degree of remaining
  13062. variation not removed by
  13063. \begin_inset Flex Glossary Term
  13064. status open
  13065. \begin_layout Plain Layout
  13066. SVA
  13067. \end_layout
  13068. \end_inset
  13069. can still swamp the effect of interest, making it difficult to detect.
  13070. This is, of course, a major issue when the end goal is to develop a classifier
  13071. to diagnose transplant rejection from methylation data, since batch-correction
  13072. methods like
  13073. \begin_inset Flex Glossary Term
  13074. status open
  13075. \begin_layout Plain Layout
  13076. SVA
  13077. \end_layout
  13078. \end_inset
  13079. that work in a linear modeling context cannot be applied in a machine learning
  13080. context.
  13081. \end_layout
  13082. \begin_layout Standard
  13083. Currently, the source of these unwanted systematic variations in the data
  13084. is unknown.
  13085. The best solution would be to determine the cause of the variation and
  13086. eliminate it, thereby eliminating the need to model and remove that variation.
  13087. However, if this proves impractical, another option is to use
  13088. \begin_inset Flex Glossary Term
  13089. status open
  13090. \begin_layout Plain Layout
  13091. SVA
  13092. \end_layout
  13093. \end_inset
  13094. to identify probes that are highly associated with the surrogate variables
  13095. that describe the unwanted variation in the data.
  13096. These probes could be discarded prior to classifier training, in order
  13097. to maximize the chance that the training algorithm will be able to identify
  13098. highly predictive probes from those remaining.
  13099. Lastly, it is possible that some of this unwanted variation is a result
  13100. of the array-based assay being used and would be eliminated by switching
  13101. to assaying DNA methylation using bisulphite sequencing.
  13102. However, this carries the risk that the sequencing assay will have its
  13103. own set of biases that must be corrected for in a different way.
  13104. \end_layout
  13105. \begin_layout Chapter
  13106. Globin-blocking for more effective blood RNA-seq analysis in primate animal
  13107. model
  13108. \end_layout
  13109. \begin_layout Standard
  13110. \size large
  13111. Ryan C.
  13112. Thompson, Terri Gelbart, Steven R.
  13113. Head, Phillip Ordoukhanian, Courtney Mullen, Dongmei Han, Dora Berman,
  13114. Amelia Bartholomew, Norma Kenyon, Daniel R.
  13115. Salomon
  13116. \end_layout
  13117. \begin_layout Standard
  13118. \begin_inset ERT
  13119. status collapsed
  13120. \begin_layout Plain Layout
  13121. \backslash
  13122. glsresetall
  13123. \end_layout
  13124. \end_inset
  13125. \begin_inset Note Note
  13126. status collapsed
  13127. \begin_layout Plain Layout
  13128. Reintroduce all abbreviations
  13129. \end_layout
  13130. \end_inset
  13131. \end_layout
  13132. \begin_layout Standard
  13133. \begin_inset Flex TODO Note (inline)
  13134. status open
  13135. \begin_layout Plain Layout
  13136. Choose between above and the paper title: Optimizing yield of deep RNA sequencin
  13137. g for gene expression profiling by globin reduction of peripheral blood
  13138. samples from cynomolgus monkeys (
  13139. \emph on
  13140. Macaca fascicularis
  13141. \emph default
  13142. ).
  13143. \end_layout
  13144. \end_inset
  13145. \end_layout
  13146. \begin_layout Section*
  13147. Abstract
  13148. \end_layout
  13149. \begin_layout Standard
  13150. \begin_inset Flex TODO Note (inline)
  13151. status open
  13152. \begin_layout Plain Layout
  13153. If the other chapters don't get abstracts, this one probably shouldn't either.
  13154. But parts of it can be copied into the final abstract.
  13155. \end_layout
  13156. \end_inset
  13157. \end_layout
  13158. \begin_layout Paragraph
  13159. Background
  13160. \end_layout
  13161. \begin_layout Standard
  13162. Primate blood contains high concentrations of globin
  13163. \begin_inset Flex Glossary Term
  13164. status open
  13165. \begin_layout Plain Layout
  13166. mRNA
  13167. \end_layout
  13168. \end_inset
  13169. .
  13170. Globin reduction is a standard technique used to improve the expression
  13171. results obtained by DNA microarrays on RNA from blood samples.
  13172. However, with
  13173. \begin_inset Flex Glossary Term
  13174. status open
  13175. \begin_layout Plain Layout
  13176. RNA-seq
  13177. \end_layout
  13178. \end_inset
  13179. quickly replacing microarrays for many applications, the impact of globin
  13180. reduction for
  13181. \begin_inset Flex Glossary Term
  13182. status open
  13183. \begin_layout Plain Layout
  13184. RNA-seq
  13185. \end_layout
  13186. \end_inset
  13187. has not been previously studied.
  13188. Moreover, no off-the-shelf kits are available for globin reduction in nonhuman
  13189. primates.
  13190. \end_layout
  13191. \begin_layout Paragraph
  13192. Results
  13193. \end_layout
  13194. \begin_layout Standard
  13195. Here we report a protocol for
  13196. \begin_inset Flex Glossary Term
  13197. status open
  13198. \begin_layout Plain Layout
  13199. RNA-seq
  13200. \end_layout
  13201. \end_inset
  13202. in primate blood samples that uses complimentary
  13203. \begin_inset Flex Glossary Term (pl)
  13204. status open
  13205. \begin_layout Plain Layout
  13206. oligo
  13207. \end_layout
  13208. \end_inset
  13209. to block reverse transcription of the alpha and beta globin genes.
  13210. In test samples from cynomolgus monkeys (
  13211. \emph on
  13212. Macaca fascicularis
  13213. \emph default
  13214. ), this
  13215. \begin_inset Flex Glossary Term
  13216. status open
  13217. \begin_layout Plain Layout
  13218. GB
  13219. \end_layout
  13220. \end_inset
  13221. protocol approximately doubles the yield of informative (non-globin) reads
  13222. by greatly reducing the fraction of globin reads, while also improving
  13223. the consistency in sequencing depth between samples.
  13224. The increased yield enables detection of about 2000 more genes, significantly
  13225. increases the correlation in measured gene expression levels between samples,
  13226. and increases the sensitivity of differential gene expression tests.
  13227. \end_layout
  13228. \begin_layout Paragraph
  13229. Conclusions
  13230. \end_layout
  13231. \begin_layout Standard
  13232. These results show that
  13233. \begin_inset Flex Glossary Term
  13234. status open
  13235. \begin_layout Plain Layout
  13236. GB
  13237. \end_layout
  13238. \end_inset
  13239. significantly improves the cost-effectiveness of
  13240. \begin_inset Flex Glossary Term
  13241. status open
  13242. \begin_layout Plain Layout
  13243. RNA-seq
  13244. \end_layout
  13245. \end_inset
  13246. in primate blood samples by doubling the yield of useful reads, allowing
  13247. detection of more genes, and improving the precision of gene expression
  13248. measurements.
  13249. Based on these results, a globin reducing or blocking protocol is recommended
  13250. for all
  13251. \begin_inset Flex Glossary Term
  13252. status open
  13253. \begin_layout Plain Layout
  13254. RNA-seq
  13255. \end_layout
  13256. \end_inset
  13257. studies of primate blood samples.
  13258. \end_layout
  13259. \begin_layout Standard
  13260. \begin_inset ERT
  13261. status collapsed
  13262. \begin_layout Plain Layout
  13263. \backslash
  13264. glsresetall
  13265. \end_layout
  13266. \end_inset
  13267. \end_layout
  13268. \begin_layout Section
  13269. Approach
  13270. \end_layout
  13271. \begin_layout Standard
  13272. \begin_inset Note Note
  13273. status open
  13274. \begin_layout Plain Layout
  13275. Consider putting some of this in the Intro chapter
  13276. \end_layout
  13277. \begin_layout Itemize
  13278. Cynomolgus monkeys as a model organism
  13279. \end_layout
  13280. \begin_deeper
  13281. \begin_layout Itemize
  13282. Highly related to humans
  13283. \end_layout
  13284. \begin_layout Itemize
  13285. Small size and short life cycle - good research animal
  13286. \end_layout
  13287. \begin_layout Itemize
  13288. Genomics resources still in development
  13289. \end_layout
  13290. \end_deeper
  13291. \begin_layout Itemize
  13292. Inadequacy of existing blood RNA-seq protocols
  13293. \end_layout
  13294. \begin_deeper
  13295. \begin_layout Itemize
  13296. Existing protocols use a separate globin pulldown step, slowing down processing
  13297. \end_layout
  13298. \end_deeper
  13299. \end_inset
  13300. \end_layout
  13301. \begin_layout Standard
  13302. Increasingly, researchers are turning to
  13303. \begin_inset Flex Glossary Term
  13304. status open
  13305. \begin_layout Plain Layout
  13306. RNA-seq
  13307. \end_layout
  13308. \end_inset
  13309. in preference to expression microarrays for analysis of whole transcriptome
  13310. gene expression
  13311. \begin_inset CommandInset citation
  13312. LatexCommand cite
  13313. key "Mutz2012"
  13314. literal "false"
  13315. \end_inset
  13316. .
  13317. The advantages are even greater for study of model organisms with no well-estab
  13318. lished array platforms available, such as the cynomolgus monkey (
  13319. \emph on
  13320. Macaca fascicularis
  13321. \emph default
  13322. ).
  13323. High fractions of globin
  13324. \begin_inset Flex Glossary Term
  13325. status open
  13326. \begin_layout Plain Layout
  13327. mRNA
  13328. \end_layout
  13329. \end_inset
  13330. are naturally present in mammalian peripheral blood samples (up to 70%
  13331. of total
  13332. \begin_inset Flex Glossary Term
  13333. status open
  13334. \begin_layout Plain Layout
  13335. mRNA
  13336. \end_layout
  13337. \end_inset
  13338. ) and these are known to interfere with the results of array-based expression
  13339. profiling
  13340. \begin_inset CommandInset citation
  13341. LatexCommand cite
  13342. key "Winn2010"
  13343. literal "false"
  13344. \end_inset
  13345. .
  13346. Globin reduction is also necessary for
  13347. \begin_inset Flex Glossary Term
  13348. status open
  13349. \begin_layout Plain Layout
  13350. RNA-seq
  13351. \end_layout
  13352. \end_inset
  13353. of blood samples, though for unrelated reasons: without globin reduction,
  13354. many
  13355. \begin_inset Flex Glossary Term
  13356. status open
  13357. \begin_layout Plain Layout
  13358. RNA-seq
  13359. \end_layout
  13360. \end_inset
  13361. reads will be derived from the globin genes, leaving fewer for the remainder
  13362. of the genes in the transcriptome.
  13363. However, existing strategies for globin reduction require an additional
  13364. step during sample preparation to deplete the population of globin transcripts
  13365. from the sample prior to reverse transcription
  13366. \begin_inset CommandInset citation
  13367. LatexCommand cite
  13368. key "Mastrokolias2012,Choi2014,Shin2014"
  13369. literal "false"
  13370. \end_inset
  13371. .
  13372. In the present report, we evaluated globin reduction by blocking reverse
  13373. transcription of globin transcripts using custom blocking
  13374. \begin_inset Flex Glossary Term (pl)
  13375. status open
  13376. \begin_layout Plain Layout
  13377. oligo
  13378. \end_layout
  13379. \end_inset
  13380. .
  13381. We demonstrate that
  13382. \begin_inset Flex Glossary Term
  13383. status open
  13384. \begin_layout Plain Layout
  13385. GB
  13386. \end_layout
  13387. \end_inset
  13388. significantly improves the cost-effectiveness of
  13389. \begin_inset Flex Glossary Term
  13390. status open
  13391. \begin_layout Plain Layout
  13392. RNA-seq
  13393. \end_layout
  13394. \end_inset
  13395. in blood samples.
  13396. Thus, our protocol offers a significant advantage to any investigator planning
  13397. to use
  13398. \begin_inset Flex Glossary Term
  13399. status open
  13400. \begin_layout Plain Layout
  13401. RNA-seq
  13402. \end_layout
  13403. \end_inset
  13404. for gene expression profiling of nonhuman primate blood samples.
  13405. Our method can be generally applied to any species by designing complementary
  13406. \begin_inset Flex Glossary Term
  13407. status open
  13408. \begin_layout Plain Layout
  13409. oligo
  13410. \end_layout
  13411. \end_inset
  13412. blocking probes to the globin gene sequences of that species.
  13413. Indeed, any highly expressed but biologically uninformative transcripts
  13414. can also be blocked to further increase sequencing efficiency and value
  13415. \begin_inset CommandInset citation
  13416. LatexCommand cite
  13417. key "Arnaud2016"
  13418. literal "false"
  13419. \end_inset
  13420. .
  13421. \end_layout
  13422. \begin_layout Section
  13423. Methods
  13424. \end_layout
  13425. \begin_layout Subsection
  13426. Sample collection
  13427. \end_layout
  13428. \begin_layout Standard
  13429. All research reported here was done under IACUC-approved protocols at the
  13430. University of Miami and complied with all applicable federal and state
  13431. regulations and ethical principles for nonhuman primate research.
  13432. Blood draws occurred between 16
  13433. \begin_inset space ~
  13434. \end_inset
  13435. April
  13436. \begin_inset space ~
  13437. \end_inset
  13438. 2012 and 18
  13439. \begin_inset space ~
  13440. \end_inset
  13441. June
  13442. \begin_inset space ~
  13443. \end_inset
  13444. 2015.
  13445. The experimental system involved intrahepatic pancreatic islet transplantation
  13446. into Cynomolgus monkeys with induced diabetes mellitus with or without
  13447. concomitant infusion of mesenchymal stem cells.
  13448. Blood was collected at serial time points before and after transplantation
  13449. into PAXgene Blood RNA tubes (PreAnalytiX/Qiagen, Valencia, CA) at the
  13450. precise volume:volume ratio of 2.5
  13451. \begin_inset space ~
  13452. \end_inset
  13453. ml whole blood into 6.9
  13454. \begin_inset space ~
  13455. \end_inset
  13456. ml of PAX gene additive.
  13457. \end_layout
  13458. \begin_layout Subsection
  13459. Globin blocking oligonucleotide design
  13460. \end_layout
  13461. \begin_layout Standard
  13462. \begin_inset Flex TODO Note (inline)
  13463. status open
  13464. \begin_layout Plain Layout
  13465. HBA1 and HBA2 is wrong for cyno?
  13466. \end_layout
  13467. \end_inset
  13468. \end_layout
  13469. \begin_layout Standard
  13470. Four
  13471. \begin_inset Flex Glossary Term (pl)
  13472. status open
  13473. \begin_layout Plain Layout
  13474. oligo
  13475. \end_layout
  13476. \end_inset
  13477. were designed to hybridize to the
  13478. \begin_inset Formula $3^{\prime}$
  13479. \end_inset
  13480. end of the transcripts for the Cynomolgus HBA1, HBA2 and HBB genes, with
  13481. two hybridization sites for HBB and 2 sites for HBA (the chosen sites were
  13482. identical in both HBA genes).
  13483. All
  13484. \begin_inset Flex Glossary Term (pl)
  13485. status open
  13486. \begin_layout Plain Layout
  13487. oligo
  13488. \end_layout
  13489. \end_inset
  13490. were purchased from Sigma and were entirely composed of 2’O-Me bases with
  13491. a C3 spacer positioned at the
  13492. \begin_inset Formula $3^{\prime}$
  13493. \end_inset
  13494. ends to prevent any polymerase mediated primer extension.
  13495. \end_layout
  13496. \begin_layout Description
  13497. HBA1/2
  13498. \begin_inset space ~
  13499. \end_inset
  13500. site
  13501. \begin_inset space ~
  13502. \end_inset
  13503. 1: GCCCACUCAGACUUUAUUCAAAG-C3spacer
  13504. \end_layout
  13505. \begin_layout Description
  13506. HBA1/2
  13507. \begin_inset space ~
  13508. \end_inset
  13509. site
  13510. \begin_inset space ~
  13511. \end_inset
  13512. 2: GGUGCAAGGAGGGGAGGAG-C3spacer
  13513. \end_layout
  13514. \begin_layout Description
  13515. HBB
  13516. \begin_inset space ~
  13517. \end_inset
  13518. site
  13519. \begin_inset space ~
  13520. \end_inset
  13521. 1: AAUGAAAAUAAAUGUUUUUUAUUAG-C3spacer
  13522. \end_layout
  13523. \begin_layout Description
  13524. HBB
  13525. \begin_inset space ~
  13526. \end_inset
  13527. site
  13528. \begin_inset space ~
  13529. \end_inset
  13530. 2: CUCAAGGCCCUUCAUAAUAUCCC-C3spacer
  13531. \end_layout
  13532. \begin_layout Subsection
  13533. RNA-seq library preparation
  13534. \end_layout
  13535. \begin_layout Standard
  13536. Sequencing libraries were prepared with 200
  13537. \begin_inset space ~
  13538. \end_inset
  13539. ng total RNA from each sample.
  13540. Polyadenylated
  13541. \begin_inset Flex Glossary Term
  13542. status open
  13543. \begin_layout Plain Layout
  13544. mRNA
  13545. \end_layout
  13546. \end_inset
  13547. was selected from 200
  13548. \begin_inset space ~
  13549. \end_inset
  13550. ng aliquots of cynomolgus blood-derived total RNA using Ambion Dynabeads
  13551. Oligo(dT)25 beads (Invitrogen) following the manufacturer’s recommended
  13552. protocol.
  13553. PolyA selected RNA was then combined with 8
  13554. \begin_inset space ~
  13555. \end_inset
  13556. pmol of HBA1/2
  13557. \begin_inset space ~
  13558. \end_inset
  13559. (site
  13560. \begin_inset space ~
  13561. \end_inset
  13562. 1), 8
  13563. \begin_inset space ~
  13564. \end_inset
  13565. pmol of HBA1/2
  13566. \begin_inset space ~
  13567. \end_inset
  13568. (site
  13569. \begin_inset space ~
  13570. \end_inset
  13571. 2), 12
  13572. \begin_inset space ~
  13573. \end_inset
  13574. pmol of HBB
  13575. \begin_inset space ~
  13576. \end_inset
  13577. (site
  13578. \begin_inset space ~
  13579. \end_inset
  13580. 1) and 12
  13581. \begin_inset space ~
  13582. \end_inset
  13583. pmol of HBB
  13584. \begin_inset space ~
  13585. \end_inset
  13586. (site
  13587. \begin_inset space ~
  13588. \end_inset
  13589. 2)
  13590. \begin_inset Flex Glossary Term (pl)
  13591. status open
  13592. \begin_layout Plain Layout
  13593. oligo
  13594. \end_layout
  13595. \end_inset
  13596. .
  13597. In addition, 20
  13598. \begin_inset space ~
  13599. \end_inset
  13600. pmol of RT primer containing a portion of the Illumina adapter sequence
  13601. (B-oligo-dTV: GAGTTCCTTGGCACCCGAGAATTCCATTTTTTTTTTTTTTTTTTTV) and 4
  13602. \begin_inset space ~
  13603. \end_inset
  13604. \emph on
  13605. μ
  13606. \emph default
  13607. L of 5X First Strand buffer (250
  13608. \begin_inset space ~
  13609. \end_inset
  13610. mM Tris-HCl pH
  13611. \begin_inset space ~
  13612. \end_inset
  13613. 8.3, 375
  13614. \begin_inset space ~
  13615. \end_inset
  13616. mM KCl, 15
  13617. \begin_inset space ~
  13618. \end_inset
  13619. mM
  13620. \begin_inset Formula $\textrm{MgCl}_{2}$
  13621. \end_inset
  13622. ) were added in a total volume of 15
  13623. \begin_inset space ~
  13624. \end_inset
  13625. µL.
  13626. The RNA was fragmented by heating this cocktail for 3 minutes at 95°C and
  13627. then placed on ice.
  13628. This was followed by the addition of 2
  13629. \begin_inset space ~
  13630. \end_inset
  13631. µL 0.1
  13632. \begin_inset space ~
  13633. \end_inset
  13634. M DTT, 1
  13635. \begin_inset space ~
  13636. \end_inset
  13637. µL RNaseOUT, 1
  13638. \begin_inset space ~
  13639. \end_inset
  13640. µL 10
  13641. \begin_inset space ~
  13642. \end_inset
  13643. mM dNTPs 10% biotin-16 aminoallyl-
  13644. \begin_inset Formula $2^{\prime}$
  13645. \end_inset
  13646. - dUTP and 10% biotin-16 aminoallyl-
  13647. \begin_inset Formula $2^{\prime}$
  13648. \end_inset
  13649. -dCTP (TriLink Biotech, San Diego, CA), 1
  13650. \begin_inset space ~
  13651. \end_inset
  13652. µL Superscript II (200
  13653. \begin_inset space ~
  13654. \end_inset
  13655. U/µL, Thermo-Fisher).
  13656. A second “unblocked” library was prepared in the same way for each sample
  13657. but replacing the blocking
  13658. \begin_inset Flex Glossary Term (pl)
  13659. status open
  13660. \begin_layout Plain Layout
  13661. oligo
  13662. \end_layout
  13663. \end_inset
  13664. with an equivalent volume of water.
  13665. The reaction was carried out at 25°C for 15 minutes and 42°C for 40 minutes,
  13666. followed by incubation at 75°C for 10 minutes to inactivate the reverse
  13667. transcriptase.
  13668. \end_layout
  13669. \begin_layout Standard
  13670. The cDNA/RNA hybrid molecules were purified using 1.8X Ampure XP beads (Agencourt
  13671. ) following supplier’s recommended protocol.
  13672. The cDNA/RNA hybrid was eluted in 25
  13673. \begin_inset space ~
  13674. \end_inset
  13675. µL of 10
  13676. \begin_inset space ~
  13677. \end_inset
  13678. mM Tris-HCl pH
  13679. \begin_inset space ~
  13680. \end_inset
  13681. 8.0, and then bound to 25
  13682. \begin_inset space ~
  13683. \end_inset
  13684. µL of M280 Magnetic Streptavidin beads washed per recommended protocol (Thermo-F
  13685. isher).
  13686. After 30 minutes of binding, beads were washed one time in 100
  13687. \begin_inset space ~
  13688. \end_inset
  13689. µL 0.1
  13690. \begin_inset space ~
  13691. \end_inset
  13692. N NaOH to denature and remove the bound RNA, followed by two 100
  13693. \begin_inset space ~
  13694. \end_inset
  13695. µL washes with 1X TE buffer.
  13696. \end_layout
  13697. \begin_layout Standard
  13698. Subsequent attachment of the
  13699. \begin_inset Formula $5^{\prime}$
  13700. \end_inset
  13701. Illumina A adapter was performed by on-bead random primer extension of
  13702. the following sequence (A-N8 primer: TTCAGAGTTCTACAGTCCGACGATCNNNNNNNN).
  13703. Briefly, beads were resuspended in a 20
  13704. \begin_inset space ~
  13705. \end_inset
  13706. µL reaction containing 5
  13707. \begin_inset space ~
  13708. \end_inset
  13709. µM A-N8 primer, 40
  13710. \begin_inset space ~
  13711. \end_inset
  13712. mM Tris-HCl pH
  13713. \begin_inset space ~
  13714. \end_inset
  13715. 7.5, 20
  13716. \begin_inset space ~
  13717. \end_inset
  13718. mM
  13719. \begin_inset Formula $\textrm{MgCl}_{2}$
  13720. \end_inset
  13721. , 50
  13722. \begin_inset space ~
  13723. \end_inset
  13724. mM NaCl, 0.325
  13725. \begin_inset space ~
  13726. \end_inset
  13727. U/µL Sequenase
  13728. \begin_inset space ~
  13729. \end_inset
  13730. 2.0 (Affymetrix, Santa Clara, CA), 0.0025
  13731. \begin_inset space ~
  13732. \end_inset
  13733. U/µL inorganic pyrophosphatase (Affymetrix) and 300
  13734. \begin_inset space ~
  13735. \end_inset
  13736. µM each dNTP.
  13737. Reaction was incubated at 22°C for 30 minutes, then beads were washed 2
  13738. times with 1X TE buffer (200
  13739. \begin_inset space ~
  13740. \end_inset
  13741. µL).
  13742. \end_layout
  13743. \begin_layout Standard
  13744. The magnetic streptavidin beads were resuspended in 34
  13745. \begin_inset space ~
  13746. \end_inset
  13747. µL nuclease-free water and added directly to a
  13748. \begin_inset Flex Glossary Term
  13749. status open
  13750. \begin_layout Plain Layout
  13751. PCR
  13752. \end_layout
  13753. \end_inset
  13754. tube.
  13755. The two Illumina protocol-specified
  13756. \begin_inset Flex Glossary Term
  13757. status open
  13758. \begin_layout Plain Layout
  13759. PCR
  13760. \end_layout
  13761. \end_inset
  13762. primers were added at 0.53
  13763. \begin_inset space ~
  13764. \end_inset
  13765. µM (Illumina TruSeq Universal Primer 1 and Illumina TruSeq barcoded
  13766. \begin_inset Flex Glossary Term
  13767. status open
  13768. \begin_layout Plain Layout
  13769. PCR
  13770. \end_layout
  13771. \end_inset
  13772. primer 2), along with 40
  13773. \begin_inset space ~
  13774. \end_inset
  13775. µL 2X KAPA HiFi Hotstart ReadyMix (KAPA, Willmington MA) and thermocycled
  13776. as follows: starting with 98°C (2 min-hold); 15 cycles of 98°C, 20sec;
  13777. 60°C, 30sec; 72°C, 30sec; and finished with a 72°C (2 min-hold).
  13778. \end_layout
  13779. \begin_layout Standard
  13780. \begin_inset Flex Glossary Term
  13781. status open
  13782. \begin_layout Plain Layout
  13783. PCR
  13784. \end_layout
  13785. \end_inset
  13786. products were purified with 1X Ampure Beads following manufacturer’s recommende
  13787. d protocol.
  13788. Libraries were then analyzed using the Agilent TapeStation and quantitation
  13789. of desired size range was performed by “smear analysis”.
  13790. Samples were pooled in equimolar batches of 16 samples.
  13791. Pooled libraries were size selected on 2% agarose gels (E-Gel EX Agarose
  13792. Gels; Thermo-Fisher).
  13793. Products were cut between 250 and 350
  13794. \begin_inset space ~
  13795. \end_inset
  13796. bp (corresponding to insert sizes of 130 to 230
  13797. \begin_inset space ~
  13798. \end_inset
  13799. bp).
  13800. Finished library pools were then sequenced on the Illumina NextSeq500 instrumen
  13801. t with 75
  13802. \begin_inset space ~
  13803. \end_inset
  13804. bp read lengths.
  13805. \end_layout
  13806. \begin_layout Subsection
  13807. Read alignment and counting
  13808. \end_layout
  13809. \begin_layout Standard
  13810. \begin_inset ERT
  13811. status collapsed
  13812. \begin_layout Plain Layout
  13813. \backslash
  13814. emergencystretch 3em
  13815. \end_layout
  13816. \end_inset
  13817. \begin_inset Note Note
  13818. status collapsed
  13819. \begin_layout Plain Layout
  13820. Need to relax the justification parameters just for this paragraph, or else
  13821. featureCounts can break out of the margin.
  13822. \end_layout
  13823. \end_inset
  13824. \end_layout
  13825. \begin_layout Standard
  13826. Reads were aligned to the cynomolgus genome using STAR
  13827. \begin_inset CommandInset citation
  13828. LatexCommand cite
  13829. key "Dobin2013,Wilson2013"
  13830. literal "false"
  13831. \end_inset
  13832. .
  13833. Counts of uniquely mapped reads were obtained for every gene in each sample
  13834. with the
  13835. \begin_inset Flex Code
  13836. status open
  13837. \begin_layout Plain Layout
  13838. featureCounts
  13839. \end_layout
  13840. \end_inset
  13841. function from the
  13842. \begin_inset Flex Code
  13843. status open
  13844. \begin_layout Plain Layout
  13845. Rsubread
  13846. \end_layout
  13847. \end_inset
  13848. package, using each of the three possibilities for the
  13849. \begin_inset Flex Code
  13850. status open
  13851. \begin_layout Plain Layout
  13852. strandSpecific
  13853. \end_layout
  13854. \end_inset
  13855. option: sense, antisense, and unstranded
  13856. \begin_inset CommandInset citation
  13857. LatexCommand cite
  13858. key "Liao2014"
  13859. literal "false"
  13860. \end_inset
  13861. .
  13862. A few artifacts in the cynomolgus genome annotation complicated read counting.
  13863. First, no ortholog is annotated for alpha globin in the cynomolgus genome,
  13864. presumably because the human genome has two alpha globin genes with nearly
  13865. identical sequences, making the orthology relationship ambiguous.
  13866. However, two loci in the cynomolgus genome are annotated as “hemoglobin
  13867. subunit alpha-like” (LOC102136192 and LOC102136846).
  13868. LOC102136192 is annotated as a pseudogene while LOC102136846 is annotated
  13869. as protein-coding.
  13870. Our globin reduction protocol was designed to include blocking of these
  13871. two genes.
  13872. Indeed, these two genes have almost the same read counts in each library
  13873. as the properly-annotated HBB gene and much larger counts than any other
  13874. gene in the unblocked libraries, giving confidence that reads derived from
  13875. the real alpha globin are mapping to both genes.
  13876. Thus, reads from both of these loci were counted as alpha globin reads
  13877. in all further analyses.
  13878. The second artifact is a small, uncharacterized non-coding RNA gene (LOC1021365
  13879. 91), which overlaps the HBA-like gene (LOC102136192) on the opposite strand.
  13880. If counting is not performed in stranded mode (or if a non-strand-specific
  13881. sequencing protocol is used), many reads mapping to the globin gene will
  13882. be discarded as ambiguous due to their overlap with this
  13883. \begin_inset Flex Glossary Term
  13884. status open
  13885. \begin_layout Plain Layout
  13886. ncRNA
  13887. \end_layout
  13888. \end_inset
  13889. gene, resulting in significant undercounting of globin reads.
  13890. Therefore, stranded sense counts were used for all further analysis in
  13891. the present study to insure that we accurately accounted for globin transcript
  13892. reduction.
  13893. However, we note that stranded reads are not necessary for
  13894. \begin_inset Flex Glossary Term
  13895. status open
  13896. \begin_layout Plain Layout
  13897. RNA-seq
  13898. \end_layout
  13899. \end_inset
  13900. using our protocol in standard practice.
  13901. \end_layout
  13902. \begin_layout Standard
  13903. \begin_inset ERT
  13904. status collapsed
  13905. \begin_layout Plain Layout
  13906. \backslash
  13907. emergencystretch 0em
  13908. \end_layout
  13909. \end_inset
  13910. \end_layout
  13911. \begin_layout Subsection
  13912. Normalization and exploratory data analysis
  13913. \end_layout
  13914. \begin_layout Standard
  13915. Libraries were normalized by computing scaling factors using the
  13916. \begin_inset Flex Code
  13917. status open
  13918. \begin_layout Plain Layout
  13919. edgeR
  13920. \end_layout
  13921. \end_inset
  13922. package's
  13923. \begin_inset Flex Glossary Term
  13924. status open
  13925. \begin_layout Plain Layout
  13926. TMM
  13927. \end_layout
  13928. \end_inset
  13929. method
  13930. \begin_inset CommandInset citation
  13931. LatexCommand cite
  13932. key "Robinson2010"
  13933. literal "false"
  13934. \end_inset
  13935. .
  13936. \begin_inset Flex Glossary Term (Capital)
  13937. status open
  13938. \begin_layout Plain Layout
  13939. logCPM
  13940. \end_layout
  13941. \end_inset
  13942. values were calculated using the
  13943. \begin_inset Flex Code
  13944. status open
  13945. \begin_layout Plain Layout
  13946. cpm
  13947. \end_layout
  13948. \end_inset
  13949. function in
  13950. \begin_inset Flex Code
  13951. status open
  13952. \begin_layout Plain Layout
  13953. edgeR
  13954. \end_layout
  13955. \end_inset
  13956. for individual samples and
  13957. \begin_inset Flex Code
  13958. status open
  13959. \begin_layout Plain Layout
  13960. aveLogCPM
  13961. \end_layout
  13962. \end_inset
  13963. function for averages across groups of samples, using those functions’
  13964. default prior count values to avoid taking the logarithm of 0.
  13965. Genes were considered “present” if their average normalized
  13966. \begin_inset Flex Glossary Term
  13967. status open
  13968. \begin_layout Plain Layout
  13969. logCPM
  13970. \end_layout
  13971. \end_inset
  13972. values across all libraries were at least
  13973. \begin_inset Formula $-1$
  13974. \end_inset
  13975. .
  13976. Normalizing for gene length was unnecessary because the sequencing protocol
  13977. is
  13978. \begin_inset Formula $3^{\prime}$
  13979. \end_inset
  13980. -biased and hence the expected read count for each gene is related to the
  13981. transcript’s copy number but not its length.
  13982. \end_layout
  13983. \begin_layout Standard
  13984. In order to assess the effect of
  13985. \begin_inset Flex Glossary Term
  13986. status open
  13987. \begin_layout Plain Layout
  13988. GB
  13989. \end_layout
  13990. \end_inset
  13991. on reproducibility, Pearson and Spearman correlation coefficients were
  13992. computed between the
  13993. \begin_inset Flex Glossary Term
  13994. status open
  13995. \begin_layout Plain Layout
  13996. logCPM
  13997. \end_layout
  13998. \end_inset
  13999. values for every pair of libraries within the
  14000. \begin_inset Flex Glossary Term
  14001. status open
  14002. \begin_layout Plain Layout
  14003. GB
  14004. \end_layout
  14005. \end_inset
  14006. non-GB groups, and
  14007. \begin_inset Flex Code
  14008. status open
  14009. \begin_layout Plain Layout
  14010. edgeR
  14011. \end_layout
  14012. \end_inset
  14013. 's
  14014. \begin_inset Flex Code
  14015. status open
  14016. \begin_layout Plain Layout
  14017. estimateDisp
  14018. \end_layout
  14019. \end_inset
  14020. function was used to compute
  14021. \begin_inset Flex Glossary Term
  14022. status open
  14023. \begin_layout Plain Layout
  14024. NB
  14025. \end_layout
  14026. \end_inset
  14027. dispersions separately for the two groups
  14028. \begin_inset CommandInset citation
  14029. LatexCommand cite
  14030. key "Chen2014"
  14031. literal "false"
  14032. \end_inset
  14033. .
  14034. \end_layout
  14035. \begin_layout Subsection
  14036. Differential expression analysis
  14037. \end_layout
  14038. \begin_layout Standard
  14039. All tests for differential gene expression were performed using
  14040. \begin_inset Flex Code
  14041. status open
  14042. \begin_layout Plain Layout
  14043. edgeR
  14044. \end_layout
  14045. \end_inset
  14046. , by first fitting a
  14047. \begin_inset Flex Glossary Term
  14048. status open
  14049. \begin_layout Plain Layout
  14050. NB
  14051. \end_layout
  14052. \end_inset
  14053. \begin_inset Flex Glossary Term
  14054. status open
  14055. \begin_layout Plain Layout
  14056. GLM
  14057. \end_layout
  14058. \end_inset
  14059. to the counts and normalization factors and then performing a quasi-likelihood
  14060. F-test with robust estimation of outlier gene dispersions
  14061. \begin_inset CommandInset citation
  14062. LatexCommand cite
  14063. key "Lund2012,Phipson2016"
  14064. literal "false"
  14065. \end_inset
  14066. .
  14067. To investigate the effects of
  14068. \begin_inset Flex Glossary Term
  14069. status open
  14070. \begin_layout Plain Layout
  14071. GB
  14072. \end_layout
  14073. \end_inset
  14074. on each gene, an additive model was fit to the full data with coefficients
  14075. for
  14076. \begin_inset Flex Glossary Term
  14077. status open
  14078. \begin_layout Plain Layout
  14079. GB
  14080. \end_layout
  14081. \end_inset
  14082. and Sample
  14083. \begin_inset Flex Glossary Term
  14084. status open
  14085. \begin_layout Plain Layout
  14086. ID
  14087. \end_layout
  14088. \end_inset
  14089. .
  14090. To test the effect of
  14091. \begin_inset Flex Glossary Term
  14092. status open
  14093. \begin_layout Plain Layout
  14094. GB
  14095. \end_layout
  14096. \end_inset
  14097. on detection of differentially expressed genes, the
  14098. \begin_inset Flex Glossary Term
  14099. status open
  14100. \begin_layout Plain Layout
  14101. GB
  14102. \end_layout
  14103. \end_inset
  14104. samples and non-GB samples were each analyzed independently as follows:
  14105. for each animal with both a pre-transplant and a post-transplant time point
  14106. in the data set, the pre-transplant sample and the earliest post-transplant
  14107. sample were selected, and all others were excluded, yielding a pre-/post-transp
  14108. lant pair of samples for each animal (
  14109. \begin_inset Formula $N=7$
  14110. \end_inset
  14111. animals with paired samples).
  14112. These samples were analyzed for pre-transplant vs.
  14113. post-transplant differential gene expression while controlling for inter-animal
  14114. variation using an additive model with coefficients for transplant and
  14115. animal
  14116. \begin_inset Flex Glossary Term
  14117. status open
  14118. \begin_layout Plain Layout
  14119. ID
  14120. \end_layout
  14121. \end_inset
  14122. .
  14123. In all analyses, p-values were adjusted using the
  14124. \begin_inset Flex Glossary Term
  14125. status open
  14126. \begin_layout Plain Layout
  14127. BH
  14128. \end_layout
  14129. \end_inset
  14130. procedure for
  14131. \begin_inset Flex Glossary Term
  14132. status open
  14133. \begin_layout Plain Layout
  14134. FDR
  14135. \end_layout
  14136. \end_inset
  14137. control
  14138. \begin_inset CommandInset citation
  14139. LatexCommand cite
  14140. key "Benjamini1995"
  14141. literal "false"
  14142. \end_inset
  14143. .
  14144. \end_layout
  14145. \begin_layout Standard
  14146. \begin_inset Note Note
  14147. status open
  14148. \begin_layout Itemize
  14149. New blood RNA-seq protocol to block reverse transcription of globin genes
  14150. \end_layout
  14151. \begin_layout Itemize
  14152. Blood RNA-seq time course after transplants with/without MSC infusion
  14153. \end_layout
  14154. \end_inset
  14155. \end_layout
  14156. \begin_layout Section
  14157. Results
  14158. \end_layout
  14159. \begin_layout Subsection
  14160. Globin blocking yields a larger and more consistent fraction of useful reads
  14161. \end_layout
  14162. \begin_layout Standard
  14163. The objective of the present study was to validate a new protocol for deep
  14164. \begin_inset Flex Glossary Term
  14165. status open
  14166. \begin_layout Plain Layout
  14167. RNA-seq
  14168. \end_layout
  14169. \end_inset
  14170. of whole blood drawn into PaxGene tubes from cynomolgus monkeys undergoing
  14171. islet transplantation, with particular focus on minimizing the loss of
  14172. useful sequencing space to uninformative globin reads.
  14173. The details of the analysis with respect to transplant outcomes and the
  14174. impact of mesenchymal stem cell treatment will be reported in a separate
  14175. manuscript (in preparation).
  14176. To focus on the efficacy of our
  14177. \begin_inset Flex Glossary Term
  14178. status open
  14179. \begin_layout Plain Layout
  14180. GB
  14181. \end_layout
  14182. \end_inset
  14183. protocol, 37 blood samples, 16 from pre-transplant and 21 from post-transplant
  14184. time points, were each prepped once with and once without
  14185. \begin_inset Flex Glossary Term
  14186. status open
  14187. \begin_layout Plain Layout
  14188. GB
  14189. \end_layout
  14190. \end_inset
  14191. \begin_inset Flex Glossary Term (pl)
  14192. status open
  14193. \begin_layout Plain Layout
  14194. oligo
  14195. \end_layout
  14196. \end_inset
  14197. , and were then sequenced on an Illumina NextSeq500 instrument.
  14198. The number of reads aligning to each gene in the cynomolgus genome was
  14199. counted.
  14200. Table
  14201. \begin_inset CommandInset ref
  14202. LatexCommand ref
  14203. reference "tab:Fractions-of-reads"
  14204. plural "false"
  14205. caps "false"
  14206. noprefix "false"
  14207. \end_inset
  14208. summarizes the distribution of read fractions among the
  14209. \begin_inset Flex Glossary Term
  14210. status open
  14211. \begin_layout Plain Layout
  14212. GB
  14213. \end_layout
  14214. \end_inset
  14215. and non-GB libraries.
  14216. In the libraries with no
  14217. \begin_inset Flex Glossary Term
  14218. status open
  14219. \begin_layout Plain Layout
  14220. GB
  14221. \end_layout
  14222. \end_inset
  14223. , globin reads made up an average of 44.6% of total input reads, while reads
  14224. assigned to all other genes made up an average of 26.3%.
  14225. The remaining reads either aligned to intergenic regions (that include
  14226. long non-coding RNAs) or did not align with any annotated transcripts in
  14227. the current build of the cynomolgus genome.
  14228. In the
  14229. \begin_inset Flex Glossary Term
  14230. status open
  14231. \begin_layout Plain Layout
  14232. GB
  14233. \end_layout
  14234. \end_inset
  14235. libraries, globin reads made up only 3.48% and reads assigned to all other
  14236. genes increased to 50.4%.
  14237. Thus,
  14238. \begin_inset Flex Glossary Term
  14239. status open
  14240. \begin_layout Plain Layout
  14241. GB
  14242. \end_layout
  14243. \end_inset
  14244. resulted in a 92.2% reduction in globin reads and a 91.6% increase in yield
  14245. of useful non-globin reads.
  14246. \end_layout
  14247. \begin_layout Standard
  14248. \begin_inset ERT
  14249. status open
  14250. \begin_layout Plain Layout
  14251. \backslash
  14252. afterpage{
  14253. \end_layout
  14254. \begin_layout Plain Layout
  14255. \backslash
  14256. begin{landscape}
  14257. \end_layout
  14258. \end_inset
  14259. \end_layout
  14260. \begin_layout Standard
  14261. \begin_inset Float table
  14262. placement p
  14263. wide false
  14264. sideways false
  14265. status collapsed
  14266. \begin_layout Plain Layout
  14267. \align center
  14268. \begin_inset Tabular
  14269. <lyxtabular version="3" rows="4" columns="7">
  14270. <features tabularvalignment="middle">
  14271. <column alignment="center" valignment="top">
  14272. <column alignment="center" valignment="top">
  14273. <column alignment="center" valignment="top">
  14274. <column alignment="center" valignment="top">
  14275. <column alignment="center" valignment="top">
  14276. <column alignment="center" valignment="top">
  14277. <column alignment="center" valignment="top">
  14278. <row>
  14279. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  14280. \begin_inset Text
  14281. \begin_layout Plain Layout
  14282. \end_layout
  14283. \end_inset
  14284. </cell>
  14285. <cell multicolumn="1" alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  14286. \begin_inset Text
  14287. \begin_layout Plain Layout
  14288. \family roman
  14289. \series medium
  14290. \shape up
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  14299. \color none
  14300. Percent of Total Reads
  14301. \end_layout
  14302. \end_inset
  14303. </cell>
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  14305. \begin_inset Text
  14306. \begin_layout Plain Layout
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  14312. \begin_layout Plain Layout
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  14317. \begin_inset Text
  14318. \begin_layout Plain Layout
  14319. \end_layout
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  14323. \begin_inset Text
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  14336. \color none
  14337. Percent of Genic Reads
  14338. \end_layout
  14339. \end_inset
  14340. </cell>
  14341. <cell multicolumn="2" alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
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  14349. <cell alignment="center" valignment="top" bottomline="true" leftline="true" usebox="none">
  14350. \begin_inset Text
  14351. \begin_layout Plain Layout
  14352. GB
  14353. \end_layout
  14354. \end_inset
  14355. </cell>
  14356. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  14357. \begin_inset Text
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  14365. \strikeout off
  14366. \xout off
  14367. \uuline off
  14368. \uwave off
  14369. \noun off
  14370. \color none
  14371. Non-globin Reads
  14372. \end_layout
  14373. \end_inset
  14374. </cell>
  14375. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  14376. \begin_inset Text
  14377. \begin_layout Plain Layout
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  14384. \strikeout off
  14385. \xout off
  14386. \uuline off
  14387. \uwave off
  14388. \noun off
  14389. \color none
  14390. Globin Reads
  14391. \end_layout
  14392. \end_inset
  14393. </cell>
  14394. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  14395. \begin_inset Text
  14396. \begin_layout Plain Layout
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  14404. \xout off
  14405. \uuline off
  14406. \uwave off
  14407. \noun off
  14408. \color none
  14409. All Genic Reads
  14410. \end_layout
  14411. \end_inset
  14412. </cell>
  14413. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  14414. \begin_inset Text
  14415. \begin_layout Plain Layout
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  14420. \emph off
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  14422. \strikeout off
  14423. \xout off
  14424. \uuline off
  14425. \uwave off
  14426. \noun off
  14427. \color none
  14428. All Aligned Reads
  14429. \end_layout
  14430. \end_inset
  14431. </cell>
  14432. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  14433. \begin_inset Text
  14434. \begin_layout Plain Layout
  14435. \family roman
  14436. \series medium
  14437. \shape up
  14438. \size normal
  14439. \emph off
  14440. \bar no
  14441. \strikeout off
  14442. \xout off
  14443. \uuline off
  14444. \uwave off
  14445. \noun off
  14446. \color none
  14447. Non-globin Reads
  14448. \end_layout
  14449. \end_inset
  14450. </cell>
  14451. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" rightline="true" usebox="none">
  14452. \begin_inset Text
  14453. \begin_layout Plain Layout
  14454. \family roman
  14455. \series medium
  14456. \shape up
  14457. \size normal
  14458. \emph off
  14459. \bar no
  14460. \strikeout off
  14461. \xout off
  14462. \uuline off
  14463. \uwave off
  14464. \noun off
  14465. \color none
  14466. Globin Reads
  14467. \end_layout
  14468. \end_inset
  14469. </cell>
  14470. </row>
  14471. <row>
  14472. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  14473. \begin_inset Text
  14474. \begin_layout Plain Layout
  14475. \family roman
  14476. \series medium
  14477. \shape up
  14478. \size normal
  14479. \emph off
  14480. \bar no
  14481. \strikeout off
  14482. \xout off
  14483. \uuline off
  14484. \uwave off
  14485. \noun off
  14486. \color none
  14487. Yes
  14488. \end_layout
  14489. \end_inset
  14490. </cell>
  14491. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  14492. \begin_inset Text
  14493. \begin_layout Plain Layout
  14494. \family roman
  14495. \series medium
  14496. \shape up
  14497. \size normal
  14498. \emph off
  14499. \bar no
  14500. \strikeout off
  14501. \xout off
  14502. \uuline off
  14503. \uwave off
  14504. \noun off
  14505. \color none
  14506. 50.4% ± 6.82
  14507. \end_layout
  14508. \end_inset
  14509. </cell>
  14510. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  14511. \begin_inset Text
  14512. \begin_layout Plain Layout
  14513. \family roman
  14514. \series medium
  14515. \shape up
  14516. \size normal
  14517. \emph off
  14518. \bar no
  14519. \strikeout off
  14520. \xout off
  14521. \uuline off
  14522. \uwave off
  14523. \noun off
  14524. \color none
  14525. 3.48% ± 2.94
  14526. \end_layout
  14527. \end_inset
  14528. </cell>
  14529. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  14530. \begin_inset Text
  14531. \begin_layout Plain Layout
  14532. \family roman
  14533. \series medium
  14534. \shape up
  14535. \size normal
  14536. \emph off
  14537. \bar no
  14538. \strikeout off
  14539. \xout off
  14540. \uuline off
  14541. \uwave off
  14542. \noun off
  14543. \color none
  14544. 53.9% ± 6.81
  14545. \end_layout
  14546. \end_inset
  14547. </cell>
  14548. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  14549. \begin_inset Text
  14550. \begin_layout Plain Layout
  14551. \family roman
  14552. \series medium
  14553. \shape up
  14554. \size normal
  14555. \emph off
  14556. \bar no
  14557. \strikeout off
  14558. \xout off
  14559. \uuline off
  14560. \uwave off
  14561. \noun off
  14562. \color none
  14563. 89.7% ± 2.40
  14564. \end_layout
  14565. \end_inset
  14566. </cell>
  14567. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  14568. \begin_inset Text
  14569. \begin_layout Plain Layout
  14570. \family roman
  14571. \series medium
  14572. \shape up
  14573. \size normal
  14574. \emph off
  14575. \bar no
  14576. \strikeout off
  14577. \xout off
  14578. \uuline off
  14579. \uwave off
  14580. \noun off
  14581. \color none
  14582. 93.5% ± 5.25
  14583. \end_layout
  14584. \end_inset
  14585. </cell>
  14586. <cell alignment="center" valignment="top" topline="true" leftline="true" rightline="true" usebox="none">
  14587. \begin_inset Text
  14588. \begin_layout Plain Layout
  14589. \family roman
  14590. \series medium
  14591. \shape up
  14592. \size normal
  14593. \emph off
  14594. \bar no
  14595. \strikeout off
  14596. \xout off
  14597. \uuline off
  14598. \uwave off
  14599. \noun off
  14600. \color none
  14601. 6.49% ± 5.25
  14602. \end_layout
  14603. \end_inset
  14604. </cell>
  14605. </row>
  14606. <row>
  14607. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  14608. \begin_inset Text
  14609. \begin_layout Plain Layout
  14610. \family roman
  14611. \series medium
  14612. \shape up
  14613. \size normal
  14614. \emph off
  14615. \bar no
  14616. \strikeout off
  14617. \xout off
  14618. \uuline off
  14619. \uwave off
  14620. \noun off
  14621. \color none
  14622. No
  14623. \end_layout
  14624. \end_inset
  14625. </cell>
  14626. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  14627. \begin_inset Text
  14628. \begin_layout Plain Layout
  14629. \family roman
  14630. \series medium
  14631. \shape up
  14632. \size normal
  14633. \emph off
  14634. \bar no
  14635. \strikeout off
  14636. \xout off
  14637. \uuline off
  14638. \uwave off
  14639. \noun off
  14640. \color none
  14641. 26.3% ± 8.95
  14642. \end_layout
  14643. \end_inset
  14644. </cell>
  14645. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  14646. \begin_inset Text
  14647. \begin_layout Plain Layout
  14648. \family roman
  14649. \series medium
  14650. \shape up
  14651. \size normal
  14652. \emph off
  14653. \bar no
  14654. \strikeout off
  14655. \xout off
  14656. \uuline off
  14657. \uwave off
  14658. \noun off
  14659. \color none
  14660. 44.6% ± 16.6
  14661. \end_layout
  14662. \end_inset
  14663. </cell>
  14664. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  14665. \begin_inset Text
  14666. \begin_layout Plain Layout
  14667. \family roman
  14668. \series medium
  14669. \shape up
  14670. \size normal
  14671. \emph off
  14672. \bar no
  14673. \strikeout off
  14674. \xout off
  14675. \uuline off
  14676. \uwave off
  14677. \noun off
  14678. \color none
  14679. 70.1% ± 9.38
  14680. \end_layout
  14681. \end_inset
  14682. </cell>
  14683. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  14684. \begin_inset Text
  14685. \begin_layout Plain Layout
  14686. \family roman
  14687. \series medium
  14688. \shape up
  14689. \size normal
  14690. \emph off
  14691. \bar no
  14692. \strikeout off
  14693. \xout off
  14694. \uuline off
  14695. \uwave off
  14696. \noun off
  14697. \color none
  14698. 90.7% ± 5.16
  14699. \end_layout
  14700. \end_inset
  14701. </cell>
  14702. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" usebox="none">
  14703. \begin_inset Text
  14704. \begin_layout Plain Layout
  14705. \family roman
  14706. \series medium
  14707. \shape up
  14708. \size normal
  14709. \emph off
  14710. \bar no
  14711. \strikeout off
  14712. \xout off
  14713. \uuline off
  14714. \uwave off
  14715. \noun off
  14716. \color none
  14717. 38.8% ± 17.1
  14718. \end_layout
  14719. \end_inset
  14720. </cell>
  14721. <cell alignment="center" valignment="top" topline="true" bottomline="true" leftline="true" rightline="true" usebox="none">
  14722. \begin_inset Text
  14723. \begin_layout Plain Layout
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  14725. \series medium
  14726. \shape up
  14727. \size normal
  14728. \emph off
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  14730. \strikeout off
  14731. \xout off
  14732. \uuline off
  14733. \uwave off
  14734. \noun off
  14735. \color none
  14736. 61.2% ± 17.1
  14737. \end_layout
  14738. \end_inset
  14739. </cell>
  14740. </row>
  14741. </lyxtabular>
  14742. \end_inset
  14743. \end_layout
  14744. \begin_layout Plain Layout
  14745. \begin_inset Caption Standard
  14746. \begin_layout Plain Layout
  14747. \begin_inset Argument 1
  14748. status collapsed
  14749. \begin_layout Plain Layout
  14750. Fractions of reads mapping to genomic features in GB and non-GB samples.
  14751. \end_layout
  14752. \end_inset
  14753. \begin_inset CommandInset label
  14754. LatexCommand label
  14755. name "tab:Fractions-of-reads"
  14756. \end_inset
  14757. \series bold
  14758. Fractions of reads mapping to genomic features in GB and non-GB samples.
  14759. \series default
  14760. All values are given as mean ± standard deviation.
  14761. \end_layout
  14762. \end_inset
  14763. \end_layout
  14764. \end_inset
  14765. \end_layout
  14766. \begin_layout Standard
  14767. \begin_inset ERT
  14768. status open
  14769. \begin_layout Plain Layout
  14770. \backslash
  14771. end{landscape}
  14772. \end_layout
  14773. \begin_layout Plain Layout
  14774. }
  14775. \end_layout
  14776. \end_inset
  14777. \end_layout
  14778. \begin_layout Standard
  14779. This reduction is not quite as efficient as the previous analysis showed
  14780. for human samples by DeepSAGE (<0.4% globin reads after globin reduction)
  14781. \begin_inset CommandInset citation
  14782. LatexCommand cite
  14783. key "Mastrokolias2012"
  14784. literal "false"
  14785. \end_inset
  14786. .
  14787. Nonetheless, this degree of globin reduction is sufficient to nearly double
  14788. the yield of useful reads.
  14789. Thus,
  14790. \begin_inset Flex Glossary Term
  14791. status open
  14792. \begin_layout Plain Layout
  14793. GB
  14794. \end_layout
  14795. \end_inset
  14796. cuts the required sequencing effort (and costs) to achieve a target coverage
  14797. depth by almost 50%.
  14798. Consistent with this near doubling of yield, the average difference in
  14799. un-normalized
  14800. \begin_inset Flex Glossary Term
  14801. status open
  14802. \begin_layout Plain Layout
  14803. logCPM
  14804. \end_layout
  14805. \end_inset
  14806. across all genes between the
  14807. \begin_inset Flex Glossary Term
  14808. status open
  14809. \begin_layout Plain Layout
  14810. GB
  14811. \end_layout
  14812. \end_inset
  14813. libraries and non-GB libraries is approximately 1 (mean = 1.01, median =
  14814. 1.08), an overall 2-fold increase.
  14815. Un-normalized values are used here because the
  14816. \begin_inset Flex Glossary Term
  14817. status open
  14818. \begin_layout Plain Layout
  14819. TMM
  14820. \end_layout
  14821. \end_inset
  14822. normalization correctly identifies this 2-fold difference as biologically
  14823. irrelevant and removes it.
  14824. \end_layout
  14825. \begin_layout Standard
  14826. Another important aspect is that the standard deviations in Table
  14827. \begin_inset CommandInset ref
  14828. LatexCommand ref
  14829. reference "tab:Fractions-of-reads"
  14830. plural "false"
  14831. caps "false"
  14832. noprefix "false"
  14833. \end_inset
  14834. are uniformly smaller in the
  14835. \begin_inset Flex Glossary Term
  14836. status open
  14837. \begin_layout Plain Layout
  14838. GB
  14839. \end_layout
  14840. \end_inset
  14841. samples than the non-GB ones, indicating much greater consistency of yield.
  14842. This is best seen in the percentage of non-globin reads as a fraction of
  14843. total reads aligned to annotated genes (genic reads).
  14844. For the non-GB samples, this measure ranges from 10.9% to 80.9%, while for
  14845. the
  14846. \begin_inset Flex Glossary Term
  14847. status open
  14848. \begin_layout Plain Layout
  14849. GB
  14850. \end_layout
  14851. \end_inset
  14852. samples it ranges from 81.9% to 99.9% (Figure
  14853. \begin_inset CommandInset ref
  14854. LatexCommand ref
  14855. reference "fig:Fraction-of-genic-reads"
  14856. plural "false"
  14857. caps "false"
  14858. noprefix "false"
  14859. \end_inset
  14860. \begin_inset Float figure
  14861. wide false
  14862. sideways false
  14863. status collapsed
  14864. \begin_layout Plain Layout
  14865. \align center
  14866. \begin_inset Graphics
  14867. filename graphics/globin-paper/figure1-globin-fractions.pdf
  14868. lyxscale 50
  14869. width 100col%
  14870. groupId colfullwidth
  14871. \end_inset
  14872. \end_layout
  14873. \begin_layout Plain Layout
  14874. \begin_inset Caption Standard
  14875. \begin_layout Plain Layout
  14876. \begin_inset Argument 1
  14877. status collapsed
  14878. \begin_layout Plain Layout
  14879. Fraction of genic reads in each sample aligned to non-globin genes, with
  14880. and without GB.
  14881. \end_layout
  14882. \end_inset
  14883. \begin_inset CommandInset label
  14884. LatexCommand label
  14885. name "fig:Fraction-of-genic-reads"
  14886. \end_inset
  14887. \series bold
  14888. Fraction of genic reads in each sample aligned to non-globin genes, with
  14889. and without GB.
  14890. \series default
  14891. All reads in each sequencing library were aligned to the cyno genome, and
  14892. the number of reads uniquely aligning to each gene was counted.
  14893. For each sample, counts were summed separately for all globin genes and
  14894. for the remainder of the genes (non-globin genes), and the fraction of
  14895. genic reads aligned to non-globin genes was computed.
  14896. Each point represents an individual sample.
  14897. Gray + signs indicate the means for globin-blocked libraries and unblocked
  14898. libraries.
  14899. The overall distribution for each group is represented as a notched box
  14900. plot.
  14901. Points are randomly spread vertically to avoid excessive overlapping.
  14902. \end_layout
  14903. \end_inset
  14904. \end_layout
  14905. \end_inset
  14906. \begin_inset Note Note
  14907. status open
  14908. \begin_layout Plain Layout
  14909. Float lost issues
  14910. \end_layout
  14911. \end_inset
  14912. ).
  14913. This means that for applications where it is critical that each sample
  14914. achieve a specified minimum coverage in order to provide useful information,
  14915. it would be necessary to budget up to 10 times the sequencing depth per
  14916. sample without
  14917. \begin_inset Flex Glossary Term
  14918. status open
  14919. \begin_layout Plain Layout
  14920. GB
  14921. \end_layout
  14922. \end_inset
  14923. , even though the average yield improvement for
  14924. \begin_inset Flex Glossary Term
  14925. status open
  14926. \begin_layout Plain Layout
  14927. GB
  14928. \end_layout
  14929. \end_inset
  14930. is only 2-fold, because every sample has a chance of being 90% globin and
  14931. 10% useful reads.
  14932. Hence, the more consistent behavior of
  14933. \begin_inset Flex Glossary Term
  14934. status open
  14935. \begin_layout Plain Layout
  14936. GB
  14937. \end_layout
  14938. \end_inset
  14939. samples makes planning an experiment easier and more efficient because
  14940. it eliminates the need to over-sequence every sample in order to guard
  14941. against the worst case of a high-globin fraction.
  14942. \end_layout
  14943. \begin_layout Subsection
  14944. Globin blocking lowers the noise floor and allows detection of about 2000
  14945. more low-expression genes
  14946. \end_layout
  14947. \begin_layout Standard
  14948. \begin_inset Flex TODO Note (inline)
  14949. status open
  14950. \begin_layout Plain Layout
  14951. Remove redundant titles from figures
  14952. \end_layout
  14953. \end_inset
  14954. \end_layout
  14955. \begin_layout Standard
  14956. Since
  14957. \begin_inset Flex Glossary Term
  14958. status open
  14959. \begin_layout Plain Layout
  14960. GB
  14961. \end_layout
  14962. \end_inset
  14963. yields more usable sequencing depth, it should also allow detection of
  14964. more genes at any given threshold.
  14965. When we looked at the distribution of average normalized
  14966. \begin_inset Flex Glossary Term
  14967. status open
  14968. \begin_layout Plain Layout
  14969. logCPM
  14970. \end_layout
  14971. \end_inset
  14972. values across all libraries for genes with at least one read assigned to
  14973. them, we observed the expected bimodal distribution, with a high-abundance
  14974. "signal" peak representing detected genes and a low-abundance "noise" peak
  14975. representing genes whose read count did not rise above the noise floor
  14976. (Figure
  14977. \begin_inset CommandInset ref
  14978. LatexCommand ref
  14979. reference "fig:logcpm-dists"
  14980. plural "false"
  14981. caps "false"
  14982. noprefix "false"
  14983. \end_inset
  14984. ).
  14985. Consistent with the 2-fold increase in raw counts assigned to non-globin
  14986. genes, the signal peak for
  14987. \begin_inset Flex Glossary Term
  14988. status open
  14989. \begin_layout Plain Layout
  14990. GB
  14991. \end_layout
  14992. \end_inset
  14993. samples is shifted to the right relative to the non-GB signal peak.
  14994. When all the samples are normalized together, this difference is normalized
  14995. out, lining up the signal peaks, and this reveals that, as expected, the
  14996. noise floor for the
  14997. \begin_inset Flex Glossary Term
  14998. status open
  14999. \begin_layout Plain Layout
  15000. GB
  15001. \end_layout
  15002. \end_inset
  15003. samples is about 2-fold lower.
  15004. This greater separation between signal and noise peaks in the
  15005. \begin_inset Flex Glossary Term
  15006. status open
  15007. \begin_layout Plain Layout
  15008. GB
  15009. \end_layout
  15010. \end_inset
  15011. samples means that low-expression genes should be more easily detected
  15012. and more precisely quantified than in the non-GB samples.
  15013. \end_layout
  15014. \begin_layout Standard
  15015. \begin_inset Float figure
  15016. wide false
  15017. sideways false
  15018. status open
  15019. \begin_layout Plain Layout
  15020. \align center
  15021. \begin_inset Graphics
  15022. filename graphics/globin-paper/figure2-aveLogCPM-colored.pdf
  15023. lyxscale 50
  15024. height 60theight%
  15025. \end_inset
  15026. \end_layout
  15027. \begin_layout Plain Layout
  15028. \begin_inset Caption Standard
  15029. \begin_layout Plain Layout
  15030. \begin_inset Argument 1
  15031. status collapsed
  15032. \begin_layout Plain Layout
  15033. Distributions of average group gene abundances when normalized separately
  15034. or together.
  15035. \end_layout
  15036. \end_inset
  15037. \begin_inset CommandInset label
  15038. LatexCommand label
  15039. name "fig:logcpm-dists"
  15040. \end_inset
  15041. \series bold
  15042. Distributions of average group gene abundances when normalized separately
  15043. or together.
  15044. \series default
  15045. All reads in each sequencing library were aligned to the cyno genome, and
  15046. the number of reads uniquely aligning to each gene was counted.
  15047. Genes with zero counts in all libraries were discarded.
  15048. Libraries were normalized using the TMM method.
  15049. Libraries were split into GB and non-GB groups and the average logCPM was
  15050. computed.
  15051. The distribution of average gene logCPM values was plotted for both groups
  15052. using a kernel density plot to approximate a continuous distribution.
  15053. The GB logCPM distributions are marked in red, non-GB in blue.
  15054. The black vertical line denotes the chosen detection threshold of
  15055. \begin_inset Formula $-1$
  15056. \end_inset
  15057. .
  15058. Top panel: Libraries were split into GB and non-GB groups first and normalized
  15059. separately.
  15060. Bottom panel: Libraries were all normalized together first and then split
  15061. into groups.
  15062. \end_layout
  15063. \end_inset
  15064. \end_layout
  15065. \end_inset
  15066. \end_layout
  15067. \begin_layout Standard
  15068. Based on these distributions, we selected a detection threshold of
  15069. \begin_inset Formula $-1$
  15070. \end_inset
  15071. , which is approximately the leftmost edge of the trough between the signal
  15072. and noise peaks.
  15073. This represents the most liberal possible detection threshold that doesn't
  15074. call substantial numbers of noise genes as detected.
  15075. Among the full dataset, 13429 genes were detected at this threshold, and
  15076. 22276 were not.
  15077. When considering the
  15078. \begin_inset Flex Glossary Term
  15079. status open
  15080. \begin_layout Plain Layout
  15081. GB
  15082. \end_layout
  15083. \end_inset
  15084. libraries and non-GB libraries separately and re-computing normalization
  15085. factors independently within each group, 14535 genes were detected in the
  15086. \begin_inset Flex Glossary Term
  15087. status open
  15088. \begin_layout Plain Layout
  15089. GB
  15090. \end_layout
  15091. \end_inset
  15092. libraries while only 12460 were detected in the non-GB libraries.
  15093. Thus,
  15094. \begin_inset Flex Glossary Term
  15095. status open
  15096. \begin_layout Plain Layout
  15097. GB
  15098. \end_layout
  15099. \end_inset
  15100. allowed the detection of 2000 extra genes that were buried under the noise
  15101. floor without
  15102. \begin_inset Flex Glossary Term
  15103. status open
  15104. \begin_layout Plain Layout
  15105. GB
  15106. \end_layout
  15107. \end_inset
  15108. .
  15109. This pattern of at least 2000 additional genes detected with
  15110. \begin_inset Flex Glossary Term
  15111. status open
  15112. \begin_layout Plain Layout
  15113. GB
  15114. \end_layout
  15115. \end_inset
  15116. was also consistent across a wide range of possible detection thresholds,
  15117. from -2 to 3 (see Figure
  15118. \begin_inset CommandInset ref
  15119. LatexCommand ref
  15120. reference "fig:Gene-detections"
  15121. plural "false"
  15122. caps "false"
  15123. noprefix "false"
  15124. \end_inset
  15125. ).
  15126. \end_layout
  15127. \begin_layout Standard
  15128. \begin_inset Float figure
  15129. wide false
  15130. sideways false
  15131. status open
  15132. \begin_layout Plain Layout
  15133. \align center
  15134. \begin_inset Graphics
  15135. filename graphics/globin-paper/figure3-detection.pdf
  15136. lyxscale 50
  15137. width 70col%
  15138. \end_inset
  15139. \end_layout
  15140. \begin_layout Plain Layout
  15141. \begin_inset Caption Standard
  15142. \begin_layout Plain Layout
  15143. \begin_inset Argument 1
  15144. status collapsed
  15145. \begin_layout Plain Layout
  15146. Gene detections as a function of abundance thresholds in GB and non-GB samples.
  15147. \end_layout
  15148. \end_inset
  15149. \begin_inset CommandInset label
  15150. LatexCommand label
  15151. name "fig:Gene-detections"
  15152. \end_inset
  15153. \series bold
  15154. Gene detections as a function of abundance thresholds in GB and non-GB samples.
  15155. \series default
  15156. Average logCPM was computed by separate group normalization as described
  15157. in Figure
  15158. \begin_inset CommandInset ref
  15159. LatexCommand ref
  15160. reference "fig:logcpm-dists"
  15161. plural "false"
  15162. caps "false"
  15163. noprefix "false"
  15164. \end_inset
  15165. for both the GB and non-GB groups, as well as for all samples considered
  15166. as one large group.
  15167. For each every integer threshold from
  15168. \begin_inset Formula $-2$
  15169. \end_inset
  15170. to 3, the number of genes detected at or above that logCPM threshold was
  15171. plotted for each group.
  15172. \end_layout
  15173. \end_inset
  15174. \end_layout
  15175. \end_inset
  15176. \end_layout
  15177. \begin_layout Subsection
  15178. Globin blocking does not add significant additional noise or decrease sample
  15179. quality
  15180. \end_layout
  15181. \begin_layout Standard
  15182. One potential worry is that the
  15183. \begin_inset Flex Glossary Term
  15184. status open
  15185. \begin_layout Plain Layout
  15186. GB
  15187. \end_layout
  15188. \end_inset
  15189. protocol could perturb the levels of non-globin genes.
  15190. There are two kinds of possible perturbations: systematic and random.
  15191. The former is not a major concern for detection of differential expression,
  15192. since a 2-fold change in every sample has no effect on the relative fold
  15193. change between samples.
  15194. In contrast, random perturbations would increase the noise and obscure
  15195. the signal in the dataset, reducing the capacity to detect differential
  15196. expression.
  15197. \end_layout
  15198. \begin_layout Standard
  15199. \begin_inset Flex TODO Note (inline)
  15200. status open
  15201. \begin_layout Plain Layout
  15202. Standardize on
  15203. \begin_inset Quotes eld
  15204. \end_inset
  15205. log2
  15206. \begin_inset Quotes erd
  15207. \end_inset
  15208. notation
  15209. \end_layout
  15210. \end_inset
  15211. \end_layout
  15212. \begin_layout Standard
  15213. The data do indeed show small systematic perturbations in gene levels (Figure
  15214. \begin_inset CommandInset ref
  15215. LatexCommand ref
  15216. reference "fig:MA-plot"
  15217. plural "false"
  15218. caps "false"
  15219. noprefix "false"
  15220. \end_inset
  15221. ).
  15222. Other than the 3 designated alpha and beta globin genes, two other genes
  15223. stand out as having especially large negative
  15224. \begin_inset Flex Glossary Term (pl)
  15225. status open
  15226. \begin_layout Plain Layout
  15227. logFC
  15228. \end_layout
  15229. \end_inset
  15230. : HBD and LOC1021365.
  15231. HBD, delta globin, is most likely targeted by the blocking
  15232. \begin_inset Flex Glossary Term (pl)
  15233. status open
  15234. \begin_layout Plain Layout
  15235. oligo
  15236. \end_layout
  15237. \end_inset
  15238. due to high sequence homology with the other globin genes.
  15239. LOC1021365 is the aforementioned
  15240. \begin_inset Flex Glossary Term
  15241. status open
  15242. \begin_layout Plain Layout
  15243. ncRNA
  15244. \end_layout
  15245. \end_inset
  15246. that is reverse-complementary to one of the alpha-like genes and that would
  15247. be expected to be removed during the
  15248. \begin_inset Flex Glossary Term
  15249. status open
  15250. \begin_layout Plain Layout
  15251. GB
  15252. \end_layout
  15253. \end_inset
  15254. step.
  15255. All other genes appear in a cluster centered vertically at 0, and the vast
  15256. majority of genes in this cluster show an absolute
  15257. \begin_inset Flex Glossary Term
  15258. status open
  15259. \begin_layout Plain Layout
  15260. logFC
  15261. \end_layout
  15262. \end_inset
  15263. of 0.5 or less.
  15264. Nevertheless, many of these small perturbations are still statistically
  15265. significant, indicating that the
  15266. \begin_inset Flex Glossary Term
  15267. status open
  15268. \begin_layout Plain Layout
  15269. GB
  15270. \end_layout
  15271. \end_inset
  15272. \begin_inset Flex Glossary Term (pl)
  15273. status open
  15274. \begin_layout Plain Layout
  15275. oligo
  15276. \end_layout
  15277. \end_inset
  15278. likely cause very small but non-zero systematic perturbations in measured
  15279. gene expression levels.
  15280. \end_layout
  15281. \begin_layout Standard
  15282. \begin_inset Float figure
  15283. wide false
  15284. sideways false
  15285. status open
  15286. \begin_layout Plain Layout
  15287. \align center
  15288. \begin_inset Graphics
  15289. filename graphics/globin-paper/figure4-maplot-colored.pdf
  15290. lyxscale 50
  15291. width 100col%
  15292. groupId colfullwidth
  15293. \end_inset
  15294. \end_layout
  15295. \begin_layout Plain Layout
  15296. \begin_inset Caption Standard
  15297. \begin_layout Plain Layout
  15298. \begin_inset Argument 1
  15299. status collapsed
  15300. \begin_layout Plain Layout
  15301. MA plot showing effects of GB on each gene's abundance.
  15302. \end_layout
  15303. \end_inset
  15304. \begin_inset CommandInset label
  15305. LatexCommand label
  15306. name "fig:MA-plot"
  15307. \end_inset
  15308. \series bold
  15309. MA plot showing effects of GB on each gene's abundance.
  15310. \series default
  15311. All libraries were normalized together as described in Figure
  15312. \begin_inset CommandInset ref
  15313. LatexCommand ref
  15314. reference "fig:logcpm-dists"
  15315. plural "false"
  15316. caps "false"
  15317. noprefix "false"
  15318. \end_inset
  15319. , and genes with an average logCPM below
  15320. \begin_inset Formula $-1$
  15321. \end_inset
  15322. were filtered out.
  15323. Each remaining gene was tested for differential abundance with respect
  15324. to
  15325. \begin_inset Flex Glossary Term (glstext)
  15326. status open
  15327. \begin_layout Plain Layout
  15328. GB
  15329. \end_layout
  15330. \end_inset
  15331. using
  15332. \begin_inset Flex Code
  15333. status open
  15334. \begin_layout Plain Layout
  15335. edgeR
  15336. \end_layout
  15337. \end_inset
  15338. ’s quasi-likelihood F-test, fitting a NB GLM to table of read counts in
  15339. each library.
  15340. For each gene,
  15341. \begin_inset Flex Code
  15342. status open
  15343. \begin_layout Plain Layout
  15344. edgeR
  15345. \end_layout
  15346. \end_inset
  15347. reported average logCPM, logFC, p-value, and BH-adjusted FDR.
  15348. Each gene's logFC was plotted against its logCPM, colored by FDR.
  15349. Red points are significant at
  15350. \begin_inset Formula $≤10\%$
  15351. \end_inset
  15352. FDR, and blue are not significant at that threshold.
  15353. The alpha and beta globin genes targeted for blocking are marked with large
  15354. triangles, while all other genes are represented as small points.
  15355. \end_layout
  15356. \end_inset
  15357. \end_layout
  15358. \end_inset
  15359. \end_layout
  15360. \begin_layout Standard
  15361. \begin_inset Flex TODO Note (inline)
  15362. status open
  15363. \begin_layout Plain Layout
  15364. Give these numbers the LaTeX math treatment
  15365. \end_layout
  15366. \end_inset
  15367. \end_layout
  15368. \begin_layout Standard
  15369. To evaluate the possibility of
  15370. \begin_inset Flex Glossary Term
  15371. status open
  15372. \begin_layout Plain Layout
  15373. GB
  15374. \end_layout
  15375. \end_inset
  15376. causing random perturbations and reducing sample quality, we computed the
  15377. Pearson correlation between
  15378. \begin_inset Flex Glossary Term
  15379. status open
  15380. \begin_layout Plain Layout
  15381. logCPM
  15382. \end_layout
  15383. \end_inset
  15384. values for every pair of samples with and without
  15385. \begin_inset Flex Glossary Term
  15386. status open
  15387. \begin_layout Plain Layout
  15388. GB
  15389. \end_layout
  15390. \end_inset
  15391. and plotted them against each other (Figure
  15392. \begin_inset CommandInset ref
  15393. LatexCommand ref
  15394. reference "fig:gene-abundance-correlations"
  15395. plural "false"
  15396. caps "false"
  15397. noprefix "false"
  15398. \end_inset
  15399. ).
  15400. The plot indicated that the
  15401. \begin_inset Flex Glossary Term
  15402. status open
  15403. \begin_layout Plain Layout
  15404. GB
  15405. \end_layout
  15406. \end_inset
  15407. libraries have higher sample-to-sample correlations than the non-GB libraries.
  15408. Parametric and nonparametric tests for differences between the correlations
  15409. with and without
  15410. \begin_inset Flex Glossary Term
  15411. status open
  15412. \begin_layout Plain Layout
  15413. GB
  15414. \end_layout
  15415. \end_inset
  15416. both confirmed that this difference was highly significant (2-sided paired
  15417. t-test:
  15418. \begin_inset Formula $t=37.2$
  15419. \end_inset
  15420. ,
  15421. \begin_inset Formula $d.f.=665$
  15422. \end_inset
  15423. ,
  15424. \begin_inset Formula $P\ll2.2\times10^{-16}$
  15425. \end_inset
  15426. ; 2-sided Wilcoxon sign-rank test:
  15427. \begin_inset Formula $V=2195$
  15428. \end_inset
  15429. ,
  15430. \begin_inset Formula $P\ll2.2\times10^{-16}$
  15431. \end_inset
  15432. ).
  15433. Performing the same tests on the Spearman correlations gave the same conclusion
  15434. (t-test:
  15435. \begin_inset Formula $t=26.8$
  15436. \end_inset
  15437. ,
  15438. \begin_inset Formula $d.f.=665$
  15439. \end_inset
  15440. ,
  15441. \begin_inset Formula $P\ll2.2\times10^{-16}$
  15442. \end_inset
  15443. ; sign-rank test:
  15444. \begin_inset Formula $V=8781$
  15445. \end_inset
  15446. ,
  15447. \begin_inset Formula $P\ll2.2\times10^{-16}$
  15448. \end_inset
  15449. ).
  15450. The
  15451. \begin_inset Flex Code
  15452. status open
  15453. \begin_layout Plain Layout
  15454. edgeR
  15455. \end_layout
  15456. \end_inset
  15457. package was used to compute the overall
  15458. \begin_inset Flex Glossary Term
  15459. status open
  15460. \begin_layout Plain Layout
  15461. BCV
  15462. \end_layout
  15463. \end_inset
  15464. for
  15465. \begin_inset Flex Glossary Term
  15466. status open
  15467. \begin_layout Plain Layout
  15468. GB
  15469. \end_layout
  15470. \end_inset
  15471. and non-GB libraries, and found that
  15472. \begin_inset Flex Glossary Term
  15473. status open
  15474. \begin_layout Plain Layout
  15475. GB
  15476. \end_layout
  15477. \end_inset
  15478. resulted in a negligible increase in the
  15479. \begin_inset Flex Glossary Term
  15480. status open
  15481. \begin_layout Plain Layout
  15482. BCV
  15483. \end_layout
  15484. \end_inset
  15485. (0.417 with
  15486. \begin_inset Flex Glossary Term
  15487. status open
  15488. \begin_layout Plain Layout
  15489. GB
  15490. \end_layout
  15491. \end_inset
  15492. vs.
  15493. 0.400 without).
  15494. The near equality of the
  15495. \begin_inset Flex Glossary Term
  15496. status open
  15497. \begin_layout Plain Layout
  15498. BCV
  15499. \end_layout
  15500. \end_inset
  15501. for both sets indicates that the higher correlations in the
  15502. \begin_inset Flex Glossary Term
  15503. status open
  15504. \begin_layout Plain Layout
  15505. GB
  15506. \end_layout
  15507. \end_inset
  15508. libraries are most likely a result of the increased yield of useful reads,
  15509. which reduces the contribution of Poisson counting uncertainty to the overall
  15510. variance of the
  15511. \begin_inset Flex Glossary Term
  15512. status open
  15513. \begin_layout Plain Layout
  15514. logCPM
  15515. \end_layout
  15516. \end_inset
  15517. values
  15518. \begin_inset CommandInset citation
  15519. LatexCommand cite
  15520. key "McCarthy2012"
  15521. literal "false"
  15522. \end_inset
  15523. .
  15524. This improves the precision of expression measurements and more than offsets
  15525. the negligible increase in
  15526. \begin_inset Flex Glossary Term
  15527. status open
  15528. \begin_layout Plain Layout
  15529. BCV
  15530. \end_layout
  15531. \end_inset
  15532. .
  15533. \end_layout
  15534. \begin_layout Standard
  15535. \begin_inset Float figure
  15536. wide false
  15537. sideways false
  15538. status open
  15539. \begin_layout Plain Layout
  15540. \align center
  15541. \begin_inset Graphics
  15542. filename graphics/globin-paper/figure5-corrplot.pdf
  15543. lyxscale 50
  15544. width 100col%
  15545. groupId colfullwidth
  15546. \end_inset
  15547. \end_layout
  15548. \begin_layout Plain Layout
  15549. \begin_inset Caption Standard
  15550. \begin_layout Plain Layout
  15551. \begin_inset Argument 1
  15552. status collapsed
  15553. \begin_layout Plain Layout
  15554. Comparison of inter-sample gene abundance correlations with and without
  15555. GB.
  15556. \end_layout
  15557. \end_inset
  15558. \begin_inset CommandInset label
  15559. LatexCommand label
  15560. name "fig:gene-abundance-correlations"
  15561. \end_inset
  15562. \series bold
  15563. Comparison of inter-sample gene abundance correlations with and without
  15564. GB.
  15565. \series default
  15566. All libraries were normalized together as described in Figure
  15567. \begin_inset CommandInset ref
  15568. LatexCommand ref
  15569. reference "fig:logcpm-dists"
  15570. plural "false"
  15571. caps "false"
  15572. noprefix "false"
  15573. \end_inset
  15574. , and genes with an average logCPM less than
  15575. \begin_inset Formula $-1$
  15576. \end_inset
  15577. were filtered out.
  15578. Each gene’s logCPM was computed in each library using
  15579. \begin_inset Flex Code
  15580. status open
  15581. \begin_layout Plain Layout
  15582. edgeR
  15583. \end_layout
  15584. \end_inset
  15585. 's
  15586. \begin_inset Flex Code
  15587. status open
  15588. \begin_layout Plain Layout
  15589. cpm
  15590. \end_layout
  15591. \end_inset
  15592. function.
  15593. For each pair of biological samples, the Pearson correlation between those
  15594. samples' GB libraries was plotted against the correlation between the same
  15595. samples’ non-GB libraries.
  15596. Each point represents an unique pair of samples.
  15597. The solid gray line shows a quantile-quantile plot of distribution of GB
  15598. correlations vs.
  15599. that of non-GB correlations.
  15600. The thin dashed line is the identity line, provided for reference.
  15601. \end_layout
  15602. \end_inset
  15603. \end_layout
  15604. \end_inset
  15605. \end_layout
  15606. \begin_layout Subsection
  15607. More differentially expressed genes are detected with globin blocking
  15608. \end_layout
  15609. \begin_layout Standard
  15610. To compare performance on differential gene expression tests, we took subsets
  15611. of both the
  15612. \begin_inset Flex Glossary Term
  15613. status open
  15614. \begin_layout Plain Layout
  15615. GB
  15616. \end_layout
  15617. \end_inset
  15618. and non-GB libraries with exactly one pre-transplant and one post-transplant
  15619. sample for each animal that had paired samples available for analysis (
  15620. \begin_inset Formula $N=7$
  15621. \end_inset
  15622. animals,
  15623. \begin_inset Formula $N=14$
  15624. \end_inset
  15625. samples in each subset).
  15626. The same test for pre- vs.
  15627. post-transplant differential gene expression was performed on the same
  15628. 7 pairs of samples from
  15629. \begin_inset Flex Glossary Term
  15630. status open
  15631. \begin_layout Plain Layout
  15632. GB
  15633. \end_layout
  15634. \end_inset
  15635. libraries and non-GB libraries, in each case using an
  15636. \begin_inset Flex Glossary Term
  15637. status open
  15638. \begin_layout Plain Layout
  15639. FDR
  15640. \end_layout
  15641. \end_inset
  15642. of 10% as the threshold of significance.
  15643. Out of 12,954 genes that passed the detection threshold in both subsets,
  15644. 358 were called significantly differentially expressed in the same direction
  15645. in both sets; 1063 were differentially expressed in the
  15646. \begin_inset Flex Glossary Term
  15647. status open
  15648. \begin_layout Plain Layout
  15649. GB
  15650. \end_layout
  15651. \end_inset
  15652. set only; 296 were differentially expressed in the non-GB set only; 2 genes
  15653. were called significantly up in the
  15654. \begin_inset Flex Glossary Term
  15655. status open
  15656. \begin_layout Plain Layout
  15657. GB
  15658. \end_layout
  15659. \end_inset
  15660. set but significantly down in the non-GB set; and the remaining 11,235
  15661. were not called differentially expressed in either set.
  15662. These data are summarized in Table
  15663. \begin_inset CommandInset ref
  15664. LatexCommand ref
  15665. reference "tab:Comparison-of-significant"
  15666. plural "false"
  15667. caps "false"
  15668. noprefix "false"
  15669. \end_inset
  15670. .
  15671. The differences in
  15672. \begin_inset Flex Glossary Term
  15673. status open
  15674. \begin_layout Plain Layout
  15675. BCV
  15676. \end_layout
  15677. \end_inset
  15678. calculated by
  15679. \begin_inset Flex Code
  15680. status open
  15681. \begin_layout Plain Layout
  15682. edgeR
  15683. \end_layout
  15684. \end_inset
  15685. for these subsets of samples were negligible (
  15686. \begin_inset Formula $\textrm{BCV}=0.302$
  15687. \end_inset
  15688. for
  15689. \begin_inset Flex Glossary Term
  15690. status open
  15691. \begin_layout Plain Layout
  15692. GB
  15693. \end_layout
  15694. \end_inset
  15695. and 0.297 for non-GB).
  15696. \end_layout
  15697. \begin_layout Standard
  15698. \begin_inset Float table
  15699. wide false
  15700. sideways false
  15701. status collapsed
  15702. \begin_layout Plain Layout
  15703. \align center
  15704. \begin_inset Tabular
  15705. <lyxtabular version="3" rows="5" columns="5">
  15706. <features tabularvalignment="middle">
  15707. <column alignment="center" valignment="top">
  15708. <column alignment="center" valignment="top">
  15709. <column alignment="center" valignment="top">
  15710. <column alignment="center" valignment="top">
  15711. <column alignment="center" valignment="top">
  15712. <row>
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  15726. \begin_inset Text
  15727. \begin_layout Plain Layout
  15728. \series bold
  15729. No Globin Blocking
  15730. \end_layout
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  15759. <cell alignment="center" valignment="top" topline="true" leftline="true" usebox="none">
  15760. \begin_inset Text
  15761. \begin_layout Plain Layout
  15762. \series bold
  15763. Up
  15764. \end_layout
  15765. \end_inset
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  15768. \begin_inset Text
  15769. \begin_layout Plain Layout
  15770. \series bold
  15771. NS
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  15776. \begin_inset Text
  15777. \begin_layout Plain Layout
  15778. \series bold
  15779. Down
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  15781. \end_inset
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  15785. <cell multirow="3" alignment="center" valignment="middle" topline="true" bottomline="true" leftline="true" usebox="none">
  15786. \begin_inset Text
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  15789. Globin-Blocking
  15790. \end_layout
  15791. \end_inset
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  15794. \begin_inset Text
  15795. \begin_layout Plain Layout
  15796. \series bold
  15797. Up
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  16000. 127
  16001. \end_layout
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  16003. </cell>
  16004. </row>
  16005. </lyxtabular>
  16006. \end_inset
  16007. \end_layout
  16008. \begin_layout Plain Layout
  16009. \begin_inset Caption Standard
  16010. \begin_layout Plain Layout
  16011. \begin_inset Argument 1
  16012. status collapsed
  16013. \begin_layout Plain Layout
  16014. Comparison of significantly differentially expressed genes with and without
  16015. globin blocking.
  16016. \end_layout
  16017. \end_inset
  16018. \begin_inset CommandInset label
  16019. LatexCommand label
  16020. name "tab:Comparison-of-significant"
  16021. \end_inset
  16022. \series bold
  16023. Comparison of significantly differentially expressed genes with and without
  16024. globin blocking.
  16025. \series default
  16026. Up, Down: Genes significantly up/down-regulated in post-transplant samples
  16027. relative to pre-transplant samples, with a false discovery rate of 10%
  16028. or less.
  16029. NS: Non-significant genes (false discovery rate greater than 10%).
  16030. \end_layout
  16031. \end_inset
  16032. \end_layout
  16033. \end_inset
  16034. \end_layout
  16035. \begin_layout Standard
  16036. The key point is that the
  16037. \begin_inset Flex Glossary Term
  16038. status open
  16039. \begin_layout Plain Layout
  16040. GB
  16041. \end_layout
  16042. \end_inset
  16043. data results in substantially more differentially expressed calls than
  16044. the non-GB data.
  16045. Since there is no gold standard for this dataset, it is impossible to be
  16046. certain whether this is due to under-calling of differential expression
  16047. in the non-GB samples or over-calling in the
  16048. \begin_inset Flex Glossary Term
  16049. status open
  16050. \begin_layout Plain Layout
  16051. GB
  16052. \end_layout
  16053. \end_inset
  16054. samples.
  16055. However, given that both datasets are derived from the same biological
  16056. samples and have nearly equal
  16057. \begin_inset Flex Glossary Term (pl)
  16058. status open
  16059. \begin_layout Plain Layout
  16060. BCV
  16061. \end_layout
  16062. \end_inset
  16063. , it is more likely that the larger number of differential expression calls
  16064. in the
  16065. \begin_inset Flex Glossary Term
  16066. status open
  16067. \begin_layout Plain Layout
  16068. GB
  16069. \end_layout
  16070. \end_inset
  16071. samples are genuine detections that were enabled by the higher sequencing
  16072. depth and measurement precision of the
  16073. \begin_inset Flex Glossary Term
  16074. status open
  16075. \begin_layout Plain Layout
  16076. GB
  16077. \end_layout
  16078. \end_inset
  16079. samples.
  16080. Note that the same set of genes was considered in both subsets, so the
  16081. larger number of differentially expressed gene calls in the
  16082. \begin_inset Flex Glossary Term
  16083. status open
  16084. \begin_layout Plain Layout
  16085. GB
  16086. \end_layout
  16087. \end_inset
  16088. data set reflects a greater sensitivity to detect significant differential
  16089. gene expression and not simply the larger total number of detected genes
  16090. in
  16091. \begin_inset Flex Glossary Term
  16092. status open
  16093. \begin_layout Plain Layout
  16094. GB
  16095. \end_layout
  16096. \end_inset
  16097. samples described earlier.
  16098. \end_layout
  16099. \begin_layout Section
  16100. Discussion
  16101. \end_layout
  16102. \begin_layout Standard
  16103. The original experience with whole blood gene expression profiling on DNA
  16104. microarrays demonstrated that the high concentration of globin transcripts
  16105. reduced the sensitivity to detect genes with relatively low expression
  16106. levels, in effect, significantly reducing the sensitivity.
  16107. To address this limitation, commercial protocols for globin reduction were
  16108. developed based on strategies to block globin transcript amplification
  16109. during labeling or physically removing globin transcripts by affinity bead
  16110. methods
  16111. \begin_inset CommandInset citation
  16112. LatexCommand cite
  16113. key "Winn2010"
  16114. literal "false"
  16115. \end_inset
  16116. .
  16117. More recently, using the latest generation of labeling protocols and arrays,
  16118. it was determined that globin reduction was no longer necessary to obtain
  16119. sufficient sensitivity to detect differential transcript expression
  16120. \begin_inset CommandInset citation
  16121. LatexCommand cite
  16122. key "NuGEN2010"
  16123. literal "false"
  16124. \end_inset
  16125. .
  16126. However, we are not aware of any publications using these currently available
  16127. protocols with the latest generation of microarrays that actually compare
  16128. the detection sensitivity with and without globin reduction.
  16129. However, in practice this has now been adopted generally primarily driven
  16130. by concerns for cost control.
  16131. The main objective of our work was to directly test the impact of globin
  16132. gene transcripts and a new
  16133. \begin_inset Flex Glossary Term
  16134. status open
  16135. \begin_layout Plain Layout
  16136. GB
  16137. \end_layout
  16138. \end_inset
  16139. protocol for application to the newest generation of differential gene
  16140. expression profiling determined using next generation sequencing.
  16141. \end_layout
  16142. \begin_layout Standard
  16143. The challenge of doing global gene expression profiling in cynomolgus monkeys
  16144. is that the current available arrays were never designed to comprehensively
  16145. cover this genome and have not been updated since the first assemblies
  16146. of the cynomolgus genome were published.
  16147. Therefore, we determined that the best strategy for peripheral blood profiling
  16148. was to perform deep
  16149. \begin_inset Flex Glossary Term
  16150. status open
  16151. \begin_layout Plain Layout
  16152. RNA-seq
  16153. \end_layout
  16154. \end_inset
  16155. and inform the workflow using the latest available genome assembly and
  16156. annotation
  16157. \begin_inset CommandInset citation
  16158. LatexCommand cite
  16159. key "Wilson2013"
  16160. literal "false"
  16161. \end_inset
  16162. .
  16163. However, it was not immediately clear whether globin reduction was necessary
  16164. for
  16165. \begin_inset Flex Glossary Term
  16166. status open
  16167. \begin_layout Plain Layout
  16168. RNA-seq
  16169. \end_layout
  16170. \end_inset
  16171. or how much improvement in efficiency or sensitivity to detect differential
  16172. gene expression would be achieved for the added cost and effort.
  16173. \end_layout
  16174. \begin_layout Standard
  16175. Existing strategies for globin reduction involve degradation or physical
  16176. removal of globin transcripts in a separate step prior to reverse transcription
  16177. \begin_inset CommandInset citation
  16178. LatexCommand cite
  16179. key "Mastrokolias2012,Choi2014,Shin2014"
  16180. literal "false"
  16181. \end_inset
  16182. .
  16183. This additional step adds significant time, complexity, and cost to sample
  16184. preparation.
  16185. Faced with the need to perform
  16186. \begin_inset Flex Glossary Term
  16187. status open
  16188. \begin_layout Plain Layout
  16189. RNA-seq
  16190. \end_layout
  16191. \end_inset
  16192. on large numbers of blood samples we sought a solution to globin reduction
  16193. that could be achieved purely by adding additional reagents during the
  16194. reverse transcription reaction.
  16195. Furthermore, we needed a globin reduction method specific to cynomolgus
  16196. globin sequences that would work an organism for which no kit is available
  16197. off the shelf.
  16198. \end_layout
  16199. \begin_layout Standard
  16200. As mentioned above, the addition of
  16201. \begin_inset Flex Glossary Term
  16202. status open
  16203. \begin_layout Plain Layout
  16204. GB
  16205. \end_layout
  16206. \end_inset
  16207. \begin_inset Flex Glossary Term (pl)
  16208. status open
  16209. \begin_layout Plain Layout
  16210. oligo
  16211. \end_layout
  16212. \end_inset
  16213. has a very small impact on measured expression levels of gene expression.
  16214. However, this is a non-issue for the purposes of differential expression
  16215. testing, since a systematic change in a gene in all samples does not affect
  16216. relative expression levels between samples.
  16217. However, we must acknowledge that simple comparisons of gene expression
  16218. data obtained by
  16219. \begin_inset Flex Glossary Term
  16220. status open
  16221. \begin_layout Plain Layout
  16222. GB
  16223. \end_layout
  16224. \end_inset
  16225. and non-GB protocols are not possible without additional normalization.
  16226. \end_layout
  16227. \begin_layout Standard
  16228. More importantly,
  16229. \begin_inset Flex Glossary Term
  16230. status open
  16231. \begin_layout Plain Layout
  16232. GB
  16233. \end_layout
  16234. \end_inset
  16235. not only nearly doubles the yield of usable reads, it also increases inter-samp
  16236. le correlation and sensitivity to detect differential gene expression relative
  16237. to the same set of samples profiled without
  16238. \begin_inset Flex Glossary Term
  16239. status open
  16240. \begin_layout Plain Layout
  16241. GB
  16242. \end_layout
  16243. \end_inset
  16244. .
  16245. In addition,
  16246. \begin_inset Flex Glossary Term
  16247. status open
  16248. \begin_layout Plain Layout
  16249. GB
  16250. \end_layout
  16251. \end_inset
  16252. does not add a significant amount of random noise to the data.
  16253. \begin_inset Flex Glossary Term (Capital)
  16254. status open
  16255. \begin_layout Plain Layout
  16256. GB
  16257. \end_layout
  16258. \end_inset
  16259. thus represents a cost-effective and low-effort way to squeeze more data
  16260. and statistical power out of the same blood samples and the same amount
  16261. of sequencing.
  16262. In conclusion,
  16263. \begin_inset Flex Glossary Term
  16264. status open
  16265. \begin_layout Plain Layout
  16266. GB
  16267. \end_layout
  16268. \end_inset
  16269. greatly increases the yield of useful
  16270. \begin_inset Flex Glossary Term
  16271. status open
  16272. \begin_layout Plain Layout
  16273. RNA-seq
  16274. \end_layout
  16275. \end_inset
  16276. reads mapping to the rest of the genome, with minimal perturbations in
  16277. the relative levels of non-globin genes.
  16278. Based on these results, globin transcript reduction using sequence-specific,
  16279. complementary blocking
  16280. \begin_inset Flex Glossary Term (pl)
  16281. status open
  16282. \begin_layout Plain Layout
  16283. oligo
  16284. \end_layout
  16285. \end_inset
  16286. is recommended for all deep
  16287. \begin_inset Flex Glossary Term
  16288. status open
  16289. \begin_layout Plain Layout
  16290. RNA-seq
  16291. \end_layout
  16292. \end_inset
  16293. of cynomolgus and other nonhuman primate blood samples.
  16294. \end_layout
  16295. \begin_layout Section
  16296. Future Directions
  16297. \end_layout
  16298. \begin_layout Standard
  16299. One drawback of the
  16300. \begin_inset Flex Glossary Term
  16301. status open
  16302. \begin_layout Plain Layout
  16303. GB
  16304. \end_layout
  16305. \end_inset
  16306. method presented in this analysis is a poor yield of genic reads, only
  16307. around 50%.
  16308. In a separate experiment, the reagent mixture was modified so as to address
  16309. this drawback, resulting in a method that produces an even better reduction
  16310. in globin reads without reducing the overall fraction of genic reads.
  16311. However, the data showing this improvement consists of only a few test
  16312. samples, so the larger data set analyzed above was chosen in order to demonstra
  16313. te the effectiveness of the method in reducing globin reads while preserving
  16314. the biological signal.
  16315. \end_layout
  16316. \begin_layout Standard
  16317. The motivation for developing a fast practical way to enrich for non-globin
  16318. reads in cyno blood samples was to enable a large-scale
  16319. \begin_inset Flex Glossary Term
  16320. status open
  16321. \begin_layout Plain Layout
  16322. RNA-seq
  16323. \end_layout
  16324. \end_inset
  16325. experiment investigating the effects of mesenchymal stem cell infusion
  16326. on blood gene expression in cynomologus transplant recipients in a time
  16327. course after transplantation.
  16328. With the
  16329. \begin_inset Flex Glossary Term
  16330. status open
  16331. \begin_layout Plain Layout
  16332. GB
  16333. \end_layout
  16334. \end_inset
  16335. method in place, the way is now clear for this experiment to proceed.
  16336. \end_layout
  16337. \begin_layout Standard
  16338. \begin_inset Note Note
  16339. status open
  16340. \begin_layout Chapter*
  16341. Future Directions
  16342. \end_layout
  16343. \begin_layout Plain Layout
  16344. \begin_inset ERT
  16345. status collapsed
  16346. \begin_layout Plain Layout
  16347. \backslash
  16348. glsresetall
  16349. \end_layout
  16350. \end_inset
  16351. \begin_inset Note Note
  16352. status collapsed
  16353. \begin_layout Plain Layout
  16354. Reintroduce all abbreviations
  16355. \end_layout
  16356. \end_inset
  16357. \end_layout
  16358. \begin_layout Plain Layout
  16359. \begin_inset Flex TODO Note (inline)
  16360. status open
  16361. \begin_layout Plain Layout
  16362. If there are any chapter-independent future directions, put them here.
  16363. Otherwise, delete this section.
  16364. \end_layout
  16365. \end_inset
  16366. \end_layout
  16367. \end_inset
  16368. \end_layout
  16369. \begin_layout Chapter
  16370. Closing remarks
  16371. \end_layout
  16372. \begin_layout Standard
  16373. \begin_inset ERT
  16374. status collapsed
  16375. \begin_layout Plain Layout
  16376. \backslash
  16377. glsresetall
  16378. \end_layout
  16379. \end_inset
  16380. \begin_inset Note Note
  16381. status collapsed
  16382. \begin_layout Plain Layout
  16383. Reintroduce all abbreviations
  16384. \end_layout
  16385. \end_inset
  16386. \end_layout
  16387. \begin_layout Standard
  16388. \align center
  16389. \begin_inset ERT
  16390. status collapsed
  16391. \begin_layout Plain Layout
  16392. % Use "References" as the title of the Bibliography
  16393. \end_layout
  16394. \begin_layout Plain Layout
  16395. \backslash
  16396. renewcommand{
  16397. \backslash
  16398. bibname}{References}
  16399. \end_layout
  16400. \end_inset
  16401. \end_layout
  16402. \begin_layout Standard
  16403. \begin_inset CommandInset bibtex
  16404. LatexCommand bibtex
  16405. btprint "btPrintCited"
  16406. bibfiles "code-refs,refs-PROCESSED"
  16407. options "bibtotoc"
  16408. \end_inset
  16409. \end_layout
  16410. \begin_layout Standard
  16411. \begin_inset Flex TODO Note (inline)
  16412. status open
  16413. \begin_layout Plain Layout
  16414. Reference URLs that span pages have clickable links that include the page
  16415. numbers and watermark.
  16416. Try to fix that.
  16417. \end_layout
  16418. \end_inset
  16419. \end_layout
  16420. \end_body
  16421. \end_document