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@@ -2782,6 +2782,16 @@ status open
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\begin_inset Caption Standard
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\begin_inset Caption Standard
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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+\begin_inset Argument 1
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+status collapsed
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+
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+\begin_layout Plain Layout
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+Example MA plot of ChIP-seq read counts in 10kb bins for two arbitrary samples.
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+\end_layout
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+
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+\end_inset
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+
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+
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\begin_inset CommandInset label
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\begin_inset CommandInset label
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LatexCommand label
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LatexCommand label
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name "fig:chipseq-norm-example"
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name "fig:chipseq-norm-example"
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@@ -3069,6 +3079,16 @@ status collapsed
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\begin_inset Caption Standard
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\begin_inset Caption Standard
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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+\begin_inset Argument 1
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+status collapsed
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+
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+\begin_layout Plain Layout
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+Example p-value histogram.
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+\end_layout
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+
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+\end_inset
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+
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\begin_inset CommandInset label
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\begin_inset CommandInset label
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LatexCommand label
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LatexCommand label
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name "fig:Example-pval-hist"
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name "fig:Example-pval-hist"
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@@ -3870,8 +3890,6 @@ status open
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\begin_inset Caption Standard
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\begin_inset Caption Standard
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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-
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-\series bold
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\begin_inset CommandInset label
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\begin_inset CommandInset label
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LatexCommand label
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LatexCommand label
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name "fig:RNA-PCA-no-batchsub"
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name "fig:RNA-PCA-no-batchsub"
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@@ -3915,8 +3933,6 @@ status open
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\begin_inset Caption Standard
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\begin_inset Caption Standard
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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-
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-\series bold
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\begin_inset CommandInset label
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\begin_inset CommandInset label
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LatexCommand label
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LatexCommand label
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name "fig:RNA-PCA-ComBat-batchsub"
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name "fig:RNA-PCA-ComBat-batchsub"
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@@ -3959,6 +3975,14 @@ name "fig:RNA-PCA"
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\series bold
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\series bold
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PCoA plots of RNA-seq data showing effect of batch correction.
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PCoA plots of RNA-seq data showing effect of batch correction.
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+
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+\series default
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+The uncorrected data (a) shows a clear separation between samples from the
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+ two batches (red and blue) dominating the first principal coordinate.
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+ After correction with ComBat (b), the two batches now have approximately
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+ the same center, and the first two principal coordinates both show separation
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+ between experimental conditions rather than batches.
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+ (Note that time points are shown in hours rather than days in these plots.)
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\end_layout
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\end_layout
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\end_inset
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\end_inset
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@@ -4011,60 +4035,6 @@ literal "false"
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for comparisons involving samples in batch 1.
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for comparisons involving samples in batch 1.
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\end_layout
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\end_layout
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-\begin_layout Standard
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-\begin_inset Float figure
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-wide false
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-sideways false
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-status collapsed
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-
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-\begin_layout Plain Layout
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-\align center
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-\begin_inset Graphics
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- filename graphics/CD4-csaw/RNA-seq/weights-vs-covars-nobcv-CROP.png
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- lyxscale 25
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- width 100col%
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- groupId colwidth-raster
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-
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-\end_inset
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-\end_layout
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-
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-\begin_layout Plain Layout
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-\begin_inset Caption Standard
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-
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-\begin_layout Plain Layout
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-\begin_inset Argument 1
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-status collapsed
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-
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-\begin_layout Plain Layout
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-RNA-seq sample weights, grouped by experimental and technical covariates.
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-\end_layout
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-
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-\end_inset
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-
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-
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-\begin_inset CommandInset label
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-LatexCommand label
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-name "fig:RNA-seq-weights-vs-covars"
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-
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-\end_inset
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-
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-
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-\series bold
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-RNA-seq sample weights, grouped by experimental and technical covariates.
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-\end_layout
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-
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-\end_inset
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-
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-\end_layout
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-\end_inset
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-\end_layout
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-
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\begin_layout Standard
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\begin_layout Standard
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In any case, the
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In any case, the
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\begin_inset Flex Glossary Term
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\begin_inset Flex Glossary Term
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@@ -4188,8 +4158,97 @@ literal "false"
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.
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.
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\end_layout
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\end_layout
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+\begin_layout Standard
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+\begin_inset Float figure
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+wide false
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+sideways false
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+status open
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+
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+\begin_layout Plain Layout
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+\align center
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+\begin_inset Graphics
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+ filename graphics/CD4-csaw/RNA-seq/weights-vs-covars-nobcv-CROP.png
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+ lyxscale 25
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+ width 100col%
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+ groupId colwidth-raster
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+
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+\end_inset
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+
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+
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+\end_layout
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+
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+\begin_layout Plain Layout
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+\begin_inset Caption Standard
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+
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+\begin_layout Plain Layout
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+\begin_inset Argument 1
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+status collapsed
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+
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+\begin_layout Plain Layout
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+RNA-seq sample weights, grouped by experimental and technical covariates.
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+\end_layout
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+
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+\end_inset
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+
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+
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+\begin_inset CommandInset label
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+LatexCommand label
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+name "fig:RNA-seq-weights-vs-covars"
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+
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+\end_inset
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+
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+
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+\series bold
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+RNA-seq sample weights, grouped by experimental and technical covariates.
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+
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+\series default
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+Inverse variance weights were estimated for each sample using
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+\begin_inset Flex Code
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+status open
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+
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+\begin_layout Plain Layout
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+limma
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+\end_layout
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+
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+\end_inset
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+
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+'s
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+\begin_inset Flex Code
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+status open
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+
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+\begin_layout Plain Layout
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+arrayWeights
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+\end_layout
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+
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+\end_inset
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+
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+ function (part of
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+\begin_inset Flex Code
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+status open
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+
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+\begin_layout Plain Layout
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+voomWithQualityWeights
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+\end_layout
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+
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+\end_inset
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+
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+).
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+ The samples were grouped by each known covariate and the distribution of
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+ weights was plotted for each group.
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+\end_layout
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+
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+\end_inset
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+
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+
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+\end_layout
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+
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+\end_inset
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+
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+
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+\end_layout
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+
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\begin_layout Subsection
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\begin_layout Subsection
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-ChIP-seq differential modification analysis
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+ChIP-seq analysis
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\end_layout
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\end_layout
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\begin_layout Standard
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\begin_layout Standard
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@@ -4331,7 +4390,15 @@ ChIP-seq
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\end_inset
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\end_inset
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- data.
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+ data
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+\begin_inset CommandInset citation
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+LatexCommand cite
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+key "Kharchenko2008,Lun2015a"
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+literal "false"
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+
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+\end_inset
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+
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+.
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Peaks were called using
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Peaks were called using
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\begin_inset Flex Code
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\begin_inset Flex Code
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status open
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status open
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@@ -4416,7 +4483,7 @@ literal "false"
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\begin_inset Float figure
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\begin_inset Float figure
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wide false
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wide false
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sideways false
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sideways false
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-status open
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+status collapsed
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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\align center
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\align center
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@@ -4429,7 +4496,7 @@ status open
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\align center
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\align center
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\begin_inset Graphics
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\begin_inset Graphics
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filename graphics/CD4-csaw/csaw/CCF-plots-noBL-PAGE2-CROP.pdf
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filename graphics/CD4-csaw/csaw/CCF-plots-noBL-PAGE2-CROP.pdf
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- lyxscale 50
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+ lyxscale 75
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height 35theight%
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height 35theight%
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groupId ccf-subfig
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groupId ccf-subfig
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@@ -4487,7 +4554,7 @@ status open
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\align center
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\align center
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\begin_inset Graphics
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\begin_inset Graphics
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filename graphics/CD4-csaw/csaw/CCF-plots-PAGE2-CROP.pdf
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filename graphics/CD4-csaw/csaw/CCF-plots-PAGE2-CROP.pdf
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- lyxscale 50
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+ lyxscale 75
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height 35theight%
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height 35theight%
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groupId ccf-subfig
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groupId ccf-subfig
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@@ -4570,6 +4637,19 @@ name "fig:CCF-master"
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\series bold
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\series bold
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Strand cross-correlation plots for ChIP-seq data, before and after blacklisting.
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Strand cross-correlation plots for ChIP-seq data, before and after blacklisting.
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+
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+\series default
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+The number of reads starting at each position in the genome was counted
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+ separately for the plus and minus strands, and then the correlation coefficient
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+ between the read start counts for both strands (cross-correlation) was
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+ computed after shifting the plus strand counts forward by a specified interval
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+ (the delay).
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+ This was repeated for every delay value from 0 to 1000, and the cross-correlati
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+on values were plotted as a function of the delay.
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+ In good quality samples, cross-correlation is maximized when the delay
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+ equals the fragment size; in poor quality samples, cross-correlation is
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+ often maximized when the delay equals the read length, an artifactual peak
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+ whose cause is not fully understood.
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\end_layout
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\end_layout
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\end_inset
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\end_inset
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@@ -4606,7 +4686,26 @@ TSS
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\end_inset
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\end_inset
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.
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.
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- For H3K4me2 and H3K4me3, this distance was about 1
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+ (Note: this analysis was performed using the original peak calls and expression
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+ values from
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+\begin_inset Flex Glossary Term
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+status open
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+
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+\begin_layout Plain Layout
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+GEO
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+\end_layout
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+
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+\end_inset
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+
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+
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+\begin_inset CommandInset citation
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+LatexCommand cite
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+key "LaMere2016"
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+literal "false"
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+
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+\end_inset
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+
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+.) For H3K4me2 and H3K4me3, this distance was about 1
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\begin_inset space ~
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\begin_inset space ~
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\end_inset
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@@ -4750,7 +4849,7 @@ noprefix "false"
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\begin_inset Float figure
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\begin_inset Float figure
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wide false
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wide false
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sideways false
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sideways false
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-status open
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+status collapsed
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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\begin_inset Float figure
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@@ -5021,7 +5120,7 @@ H3K27me3, SVs subtracted
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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\begin_inset Flex TODO Note (inline)
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\begin_inset Flex TODO Note (inline)
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-status open
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+status collapsed
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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Figure font too small
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Figure font too small
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@@ -5041,7 +5140,7 @@ status collapsed
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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PCoA plots of ChIP-seq sliding window data, before and after subtracting
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PCoA plots of ChIP-seq sliding window data, before and after subtracting
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- surrogate variables (SVs).
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+ surrogate variables.
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\end_layout
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\end_layout
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\end_inset
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\end_inset
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@@ -5057,6 +5156,23 @@ name "fig:PCoA-ChIP"
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\series bold
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\series bold
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PCoA plots of ChIP-seq sliding window data, before and after subtracting
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PCoA plots of ChIP-seq sliding window data, before and after subtracting
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surrogate variables (SVs).
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surrogate variables (SVs).
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+
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+\series default
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+For each histone mark, a PCoA plot of the first 2 principal coordinates
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+ was created before and after subtraction of SV effects.
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+ Time points are shown by color and cell type by shape, and samples from
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+ the same time point and cell type are enclosed in a shaded area to aid
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+ in visial recognition (this shaded area has no meaning on the plot).
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+ Samples of the same cell type from the same donor are connected with a
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+ line in time point order, showing the
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+\begin_inset Quotes eld
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+\end_inset
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+
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+trajectory
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+\begin_inset Quotes erd
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+\end_inset
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+
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+ of each donor's samples over time.
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\end_layout
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\end_layout
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\end_inset
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\end_inset
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@@ -5160,8 +5276,7 @@ relative coverage profile
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\end_layout
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\end_layout
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\begin_layout Subsection
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\begin_layout Subsection
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-MOFA recovers biologically relevant variation from blind analysis by correlating
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- across datasets
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+MOFA analysis of cross-dataset variation patterns
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\end_layout
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\end_layout
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\begin_layout Standard
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\begin_layout Standard
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@@ -5340,7 +5455,7 @@ status open
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\begin_inset Float figure
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\begin_inset Float figure
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wide false
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wide false
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sideways false
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sideways false
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-status open
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+status collapsed
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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\align center
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@@ -5399,12 +5514,12 @@ view
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\begin_inset Float figure
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\begin_inset Float figure
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wide false
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wide false
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sideways false
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sideways false
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+status collapsed
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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\align center
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\align center
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\begin_inset Graphics
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\begin_inset Graphics
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- filename graphics/CD4-csaw/MOFA-LF-scatter-CROP.png
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+ filename graphics/CD4-csaw/MOFA-LF-scatter-small.png
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lyxscale 25
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width 45col%
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width 45col%
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groupId mofa-subfig
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groupId mofa-subfig
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@@ -5430,8 +5545,9 @@ Scatter plots of specific pairs of MOFA latent factors.
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\series default
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\series default
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LFs 1, 4, and 5 explain substantial variation in all data sets, so they
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LFs 1, 4, and 5 explain substantial variation in all data sets, so they
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- are plotted against each other in order to reveal patterns of variation
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+ were plotted against each other in order to reveal patterns of variation
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that are shared across all data sets.
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that are shared across all data sets.
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+ These plots can be interpreted similarly to PCA and PCoA plots.
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\end_layout
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\end_layout
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\end_inset
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@@ -5480,6 +5596,11 @@ name "fig:MOFA-master"
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\series bold
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\series bold
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MOFA latent factors identify shared patterns of variation.
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MOFA latent factors identify shared patterns of variation.
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+
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+\series default
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+MOFA was used to estimate latent factors (LFs) that explain substantial
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+ variation in the RNA-seq data and the ChIP-seq data (a).
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+ Then specific LFs of interest were selected and plotted (b).
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\end_layout
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\end_layout
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\end_inset
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\end_inset
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@@ -6220,7 +6341,7 @@ PCoA plot of RNA-seq samples after ComBat batch correction.
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Each point represents an individual sample.
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Each point represents an individual sample.
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Samples with the same combination of cell type and time point are encircled
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Samples with the same combination of cell type and time point are encircled
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with a shaded region to aid in visual identification of the sample groups.
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with a shaded region to aid in visual identification of the sample groups.
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- Samples with of same cell type from the same donor are connected by lines
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+ Samples of the same cell type from the same donor are connected by lines
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to indicate the
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to indicate the
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\begin_inset Quotes eld
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\begin_inset Quotes eld
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@@ -6342,7 +6463,7 @@ H3K4me2
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-14965
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-3970
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@@ -6389,7 +6510,7 @@ H3K4me3
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-6163
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+6,163
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@@ -6398,7 +6519,7 @@ H3K4me3
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\begin_inset Text
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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-2946
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+2,946
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@@ -6436,7 +6557,7 @@ H3K27me3
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\begin_inset Text
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\begin_inset Text
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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-18139
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+18,139
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@@ -6445,7 +6566,7 @@ H3K27me3
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\begin_inset Text
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\begin_inset Text
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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-18967
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+18,967
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\end_inset
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\end_inset
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@@ -6575,6 +6696,19 @@ noprefix "false"
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histones.
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histones.
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\end_layout
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\end_layout
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+\begin_layout Standard
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+\begin_inset Flex TODO Note (inline)
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+status open
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+
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+\begin_layout Plain Layout
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+
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+\end_layout
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+
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+\end_inset
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+
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+
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+\end_layout
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+
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\begin_layout Standard
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\begin_layout Standard
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All 3 histone marks tend to occur more often near promoter regions, as shown
|
|
All 3 histone marks tend to occur more often near promoter regions, as shown
|
|
in Figure
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|
in Figure
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@@ -6663,12 +6797,11 @@ sideways false
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status open
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status open
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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-\begin_inset Flex TODO Note (inline)
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-status open
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-
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-\begin_layout Plain Layout
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-Future direction idea: Need a control: shuffle all peaks and repeat, N times.
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-\end_layout
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+\align center
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+\begin_inset Graphics
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+ filename graphics/CD4-csaw/Promoter-Peak-Distance-Profile-PAGE1-CROP.pdf
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+ lyxscale 50
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+ width 80col%
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\end_inset
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\end_inset
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@@ -6676,11 +6809,12 @@ Future direction idea: Need a control: shuffle all peaks and repeat, N times.
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\end_layout
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\end_layout
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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-\align center
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-\begin_inset Graphics
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- filename graphics/CD4-csaw/Promoter-Peak-Distance-Profile-PAGE1-CROP.pdf
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- lyxscale 50
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- width 80col%
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+\begin_inset Flex TODO Note (inline)
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+status open
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+
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+\begin_layout Plain Layout
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+Future direction idea: Need a control: shuffle all peaks and repeat, N times.
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+\end_layout
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\end_inset
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\end_inset
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@@ -6723,6 +6857,26 @@ within
|
|
\emph default
|
|
\emph default
|
|
peaks were excluded from this plot to avoid a large spike at zero that
|
|
peaks were excluded from this plot to avoid a large spike at zero that
|
|
would overshadow the rest of the distribution.
|
|
would overshadow the rest of the distribution.
|
|
|
|
+ (Note: this figure was generated using the original peak calls and expression
|
|
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+ values from
|
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+\begin_inset Flex Glossary Term
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+status open
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+
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+\begin_layout Plain Layout
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+GEO
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+\end_layout
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+
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+\end_inset
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+
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+
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+\begin_inset CommandInset citation
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+LatexCommand cite
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+key "LaMere2016"
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+literal "false"
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+
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+\end_inset
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+
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+.)
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\end_layout
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\end_layout
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\end_inset
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\end_inset
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|
@@ -6980,18 +7134,21 @@ FPKM
|
|
\end_layout
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\end_layout
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\begin_layout Standard
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\begin_layout Standard
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-\begin_inset Float figure
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-wide false
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-sideways false
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-status collapsed
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+\begin_inset ERT
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+status open
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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-\begin_inset Flex TODO Note (inline)
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-status open
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+
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+
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+\backslash
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+afterpage{
|
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+\end_layout
|
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|
\begin_layout Plain Layout
|
|
\begin_layout Plain Layout
|
|
-This figure is generated from the old analysis.
|
|
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|
- Either note that in some way or re-generate it from the new peak calls.
|
|
|
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+
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+
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+\backslash
|
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+begin{landscape}
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\end_layout
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\end_layout
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\end_inset
|
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\end_inset
|
|
@@ -6999,12 +7156,18 @@ This figure is generated from the old analysis.
|
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|
|
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|
\end_layout
|
|
\end_layout
|
|
|
|
|
|
|
|
+\begin_layout Standard
|
|
|
|
+\begin_inset Float figure
|
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+wide false
|
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+sideways false
|
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+status collapsed
|
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+
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|
\begin_layout Plain Layout
|
|
\begin_layout Plain Layout
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\align center
|
|
\align center
|
|
\begin_inset Graphics
|
|
\begin_inset Graphics
|
|
filename graphics/CD4-csaw/FPKM-by-Peak-Violin-Plots-CROP.pdf
|
|
filename graphics/CD4-csaw/FPKM-by-Peak-Violin-Plots-CROP.pdf
|
|
lyxscale 50
|
|
lyxscale 50
|
|
- width 100col%
|
|
|
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+ height 80theight%
|
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\end_inset
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\end_inset
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|
@@ -7034,11 +7197,63 @@ name "fig:fpkm-by-peak"
|
|
|
|
|
|
\series bold
|
|
\series bold
|
|
Expression distributions of genes with and without promoter peaks.
|
|
Expression distributions of genes with and without promoter peaks.
|
|
|
|
+
|
|
|
|
+\series default
|
|
|
|
+For each histone mark in each experimental condition, the average RNA-seq
|
|
|
|
+ abundance (
|
|
|
|
+\begin_inset Formula $\log_{2}$
|
|
|
|
+\end_inset
|
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+
|
|
|
|
+ FPKM) of each gene across all 4 donors was calculated.
|
|
|
|
+ Genes were grouped based on whether or not a peak was called in their promoters
|
|
|
|
+ in that condition, and the distribution of abundance values was plotted
|
|
|
|
+ for the no-peak and peak groups.
|
|
|
|
+ (Note: this figure was generated using the original peak calls and expression
|
|
|
|
+ values from
|
|
|
|
+\begin_inset Flex Glossary Term
|
|
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+status open
|
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+
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+\begin_layout Plain Layout
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+GEO
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\end_layout
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\end_inset
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\end_inset
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+
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+\begin_inset CommandInset citation
|
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+LatexCommand cite
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+key "LaMere2016"
|
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|
+literal "false"
|
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+
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+\end_inset
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+
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+.)
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+\end_layout
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+
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+\end_inset
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+
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+
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+\end_layout
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+
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+\end_inset
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+
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+
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+\end_layout
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+
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+\begin_layout Standard
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+\begin_inset ERT
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+status open
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+
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+\begin_layout Plain Layout
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+
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+
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+\backslash
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+end{landscape}
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+\end_layout
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+
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+\begin_layout Plain Layout
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+}
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\end_layout
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\end_layout
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\end_inset
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@@ -7179,7 +7394,7 @@ status open
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\begin_inset Float figure
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\begin_inset Float figure
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wide false
|
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wide false
|
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sideways false
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sideways false
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-status collapsed
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+status open
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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\align center
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\align center
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@@ -7198,15 +7413,13 @@ status collapsed
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\begin_inset Caption Standard
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\begin_inset Caption Standard
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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-
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-\series bold
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\begin_inset CommandInset label
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\begin_inset CommandInset label
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LatexCommand label
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LatexCommand label
|
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name "fig:PCoA-H3K4me2-prom"
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name "fig:PCoA-H3K4me2-prom"
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\end_inset
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\end_inset
|
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|
|
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-PCoA plot of H3K4me2 promoters, after subtracting surrogate variables
|
|
|
|
|
|
+PCoA plot of H3K4me2 promoters, after subtracting surrogate variables.
|
|
\end_layout
|
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\end_layout
|
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\end_inset
|
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\end_inset
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@@ -7224,7 +7437,7 @@ PCoA plot of H3K4me2 promoters, after subtracting surrogate variables
|
|
\begin_inset Float figure
|
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\begin_inset Float figure
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wide false
|
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wide false
|
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sideways false
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sideways false
|
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-status collapsed
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+status open
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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\align center
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\align center
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@@ -7243,15 +7456,13 @@ status collapsed
|
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\begin_inset Caption Standard
|
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\begin_inset Caption Standard
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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-
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-\series bold
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\begin_inset CommandInset label
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\begin_inset CommandInset label
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LatexCommand label
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LatexCommand label
|
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name "fig:PCoA-H3K4me3-prom"
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name "fig:PCoA-H3K4me3-prom"
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|
|
\end_inset
|
|
\end_inset
|
|
|
|
|
|
-PCoA plot of H3K4me3 promoters, after subtracting surrogate variables
|
|
|
|
|
|
+PCoA plot of H3K4me3 promoters, after subtracting surrogate variables.
|
|
\end_layout
|
|
\end_layout
|
|
|
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|
\end_inset
|
|
\end_inset
|
|
@@ -7269,7 +7480,7 @@ PCoA plot of H3K4me3 promoters, after subtracting surrogate variables
|
|
\begin_inset Float figure
|
|
\begin_inset Float figure
|
|
wide false
|
|
wide false
|
|
sideways false
|
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sideways false
|
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-status collapsed
|
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+status open
|
|
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\begin_layout Plain Layout
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|
\begin_layout Plain Layout
|
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\align center
|
|
\align center
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@@ -7288,15 +7499,13 @@ status collapsed
|
|
\begin_inset Caption Standard
|
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\begin_inset Caption Standard
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\begin_layout Plain Layout
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\begin_layout Plain Layout
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-
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-\series bold
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\begin_inset CommandInset label
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\begin_inset CommandInset label
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LatexCommand label
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LatexCommand label
|
|
name "fig:PCoA-H3K27me3-prom"
|
|
name "fig:PCoA-H3K27me3-prom"
|
|
|
|
|
|
\end_inset
|
|
\end_inset
|
|
|
|
|
|
-PCoA plot of H3K27me3 promoters, after subtracting surrogate variables
|
|
|
|
|
|
+PCoA plot of H3K27me3 promoters, after subtracting surrogate variables.
|
|
\end_layout
|
|
\end_layout
|
|
|
|
|
|
\end_inset
|
|
\end_inset
|
|
@@ -7314,7 +7523,7 @@ PCoA plot of H3K27me3 promoters, after subtracting surrogate variables
|
|
\begin_inset Float figure
|
|
\begin_inset Float figure
|
|
wide false
|
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wide false
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-RNA-seq PCoA showing principal coordinates 2 and 3.
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+RNA-seq PCoA, after ComBat batch correction, showing principal coordinates
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+ 2 and 3.
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-PCoA plots for promoter ChIP-seq and expression RNA-seq data
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+PCoA plots for promoter ChIP-seq and expression RNA-seq data.
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+
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+\series default
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+Each point represents an individual sample.
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+ Samples with the same combination of cell type and time point are encircled
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+ with a shaded region to aid in visual identification of the sample groups.
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+ Samples of the same cell type from the same donor are connected by lines
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+ to indicate the
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+\begin_inset Quotes eld
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+trajectory
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+
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+ of each donor's cells over time in PCoA space.
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-Average relative coverage for each bin in each cluster
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+Average relative coverage for each bin in each cluster.
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-Average relative coverage for each bin in each cluster
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+Average relative coverage for each bin in each cluster.
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@@ -9140,9 +9349,7 @@ name "fig:H3K27me3-neighborhood-pca"
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\end_inset
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PCA of relative coverage depth, colored by K-means cluster membership.
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PCA of relative coverage depth, colored by K-means cluster membership.
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-
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-\series default
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-Note that Cluster 6 is hidden behind all the other clusters.
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+ (Note: Cluster 6 is hidden behind all the other clusters.)
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@@ -9633,9 +9838,9 @@ Look up some more references for these histone marks being involved in memory
|
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\end_layout
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\begin_layout Standard
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-We have observed that all 3 histone marks and the gene expression data all
|
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- exhibit evidence of convergence in abundance between naïve and memory cells
|
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- by day 14 after activation (Figure
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+We observed that all 3 histone marks and the gene expression data all exhibit
|
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+ evidence of convergence in abundance between naïve and memory cells by
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+ day 14 after activation (Figure
|
|
\begin_inset CommandInset ref
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LatexCommand ref
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LatexCommand ref
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reference "fig:PCoA-promoters"
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reference "fig:PCoA-promoters"
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@@ -9710,13 +9915,13 @@ LF
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in this plot, this factor explains a substantial portion of the variance
|
|
in this plot, this factor explains a substantial portion of the variance
|
|
in all 4 data sets, indicating a coordinated pattern of variation shared
|
|
in all 4 data sets, indicating a coordinated pattern of variation shared
|
|
across all histone marks and gene expression.
|
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across all histone marks and gene expression.
|
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- This, of course, is consistent with the expectation that any naïve CD4
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+ This is consistent with the expectation that any naïve CD4
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\begin_inset Formula $^{+}$
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\begin_inset Formula $^{+}$
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- T-cells remaining at day 14 should have differentiated into memory cells
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- by that time, and should therefore have a genomic state similar to memory
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- cells.
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+ T-cells remaining at day 14 should have differentiated into memory cells
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+ by that time, and should therefore have a genomic and epigenomic state
|
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+ similar to memory cells.
|
|
This convergence is evidence that these histone marks all play an important
|
|
This convergence is evidence that these histone marks all play an important
|
|
role in the naïve-to-memory differentiation process.
|
|
role in the naïve-to-memory differentiation process.
|
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A histone mark that was not involved in naïve-to-memory differentiation
|
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A histone mark that was not involved in naïve-to-memory differentiation
|
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@@ -9829,13 +10034,28 @@ PCoA
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to reveal interesting behaviors in the data that were previously only detectabl
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to reveal interesting behaviors in the data that were previously only detectabl
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e by a detailed manual analysis.
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|
e by a detailed manual analysis.
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+ While the ideal comparison to demonstrate this convergence would be naïve
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+ cells at day 14 to memory cells at day 0, this is not feasible in this
|
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+ experimental system, since neither naïve nor memory cells are able to fully
|
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+ return to their pre-activation state, as shown by the lack of overlap between
|
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+ days 0 and 14 for either naïve or memory cells in Figure
|
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+\begin_inset CommandInset ref
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+
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+.
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@@ -9862,7 +10082,7 @@ Lamere 2016 Figure 8 “Model for the role of H3K4 methylation during CD4
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- T-cell activation.
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+Model for the role of H3K4 methylation during CD4
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-While the ideal comparison to demonstrate this convergence would be naïve
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Dependency graph of steps in reproducible workflow.
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Dependency graph of steps in reproducible workflow.
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+
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+\series default
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+The analysis flows from left to right.
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+ Arrows indicate which analysis steps depend on the output of other steps.
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@@ -11486,6 +11688,15 @@ name "fig:Sigmoid-beta-m-mapping"
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\series bold
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Sigmoid shape of the mapping between β and M values.
|
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Sigmoid shape of the mapping between β and M values.
|
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+
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+\series default
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+This mapping is monotonic and non-linear, but it is approximately linear
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+ in the neighborhood of
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+\begin_inset Formula $(\beta=0.5,M=0)$
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+\end_inset
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+.
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- The blue line is only shown in each plot if the estimate of
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+ A blue line is only shown in each plot if the estimate of
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\begin_inset Formula $\hat{\pi}_{0}$
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\end_inset
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\end_inset
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- for that p-value distribution is different from 1.
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+ for that p-value distribution is smaller than 1.
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\end_layout
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@@ -17256,19 +17467,10 @@ ADNR
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\begin_inset Flex Glossary Term (pl)
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status open
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\begin_layout Plain Layout
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M-value
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for that probe in
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for that probe in
|
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@@ -21756,7 +21958,7 @@ The challenge of doing global gene expression profiling in cynomolgus monkeys
|
|
cover this genome and have not been updated since the first assemblies
|
|
cover this genome and have not been updated since the first assemblies
|
|
of the cynomolgus genome were published.
|
|
of the cynomolgus genome were published.
|
|
Therefore, we determined that the best strategy for peripheral blood profiling
|
|
Therefore, we determined that the best strategy for peripheral blood profiling
|
|
- was to do deep
|
|
|
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+ was to perform deep
|
|
\begin_inset Flex Glossary Term
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\begin_inset Flex Glossary Term
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status open
|
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status open
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