vst: Quickly estimate dispersion trend and apply a variance...
In DESeq2: Differential gene expression analysis based on the negative binomial distribution
Description
Usage
Arguments
Value
Examples
Description
This is a wrapper for the varianceStabilizingTransformation (VST)
that provides much faster estimation of the dispersion trend used to determine
the formula for the VST. The speed-up is accomplished by
subsetting to a smaller number of genes in order to estimate this dispersion trend.
The subset of genes is chosen deterministically, to span the range
of genes' mean normalized count.
This wrapper for the VST is not blind to the experimental design:
the sample covariate information is used to estimate the global trend
of genes' dispersion values over the genes' mean normalized count.
It can be made strictly blind to experimental design by first
assigning a design of ~1 before running this function,
or by avoiding subsetting and using varianceStabilizingTransformation.
Usage
1
Arguments
object
a DESeqDataSet or a matrix of counts
blind
logical, whether to blind the transformation to the experimental
design (see varianceStabilizingTransformation)
nsub
the number of genes to subset to (default 1000)
fitType
for estimation of dispersions: this parameter
is passed on to estimateDispersions (options described there)
Value
a DESeqTranform object or a matrix of transformed, normalized counts
Examples
1
2
dds <- makeExampleDESeqDataSet(n=2000, m=20)
vsd <- vst(dds)
DESeq2 documentation built on Feb. 22, 2021, 10 a.m.
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Description Usage Arguments Value Examples
Description
This is a wrapper for the varianceStabilizingTransformation (VST)
that provides much faster estimation of the dispersion trend used to determine
the formula for the VST. The speed-up is accomplished by
subsetting to a smaller number of genes in order to estimate this dispersion trend.
The subset of genes is chosen deterministically, to span the range
of genes' mean normalized count.
This wrapper for the VST is not blind to the experimental design:
the sample covariate information is used to estimate the global trend
of genes' dispersion values over the genes' mean normalized count.
It can be made strictly blind to experimental design by first
assigning a design of ~1 before running this function,
or by avoiding subsetting and using varianceStabilizingTransformation.
Usage
1 |
Arguments
object |
a DESeqDataSet or a matrix of counts |
blind |
logical, whether to blind the transformation to the experimental
design (see |
nsub |
the number of genes to subset to (default 1000) |
fitType |
for estimation of dispersions: this parameter
is passed on to |
Value
a DESeqTranform object or a matrix of transformed, normalized counts
Examples
1 2 | dds <- makeExampleDESeqDataSet(n=2000, m=20)
vsd <- vst(dds)
|
R Package Documentation
Browse R Packages
We want your feedback!
Note that we can't provide technical support on individual packages. You should contact the package authors for that.
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