carinelegrand/RiboVIEW
Visualization, Quality and Statistics for Ribosome Profiling

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batch.effects.lm.e: Apply a linear fit to codon enrichment with a, c, g or u as...

batch.effects.lm.e: Apply a linear fit to codon enrichment with a, c, g or u as...
In carinelegrand/RiboVIEW: Visualization, Quality and Statistics for Ribosome Profiling

Description Usage Arguments Value Examples

View source: R/batch-effects.R

Description

batch.effects.lm This function takes a list of samples and their conditions as input and applies a linear fit to each of these samples' codon enrichment. Explanatory variable is successively a, c, g and u. A plot of coefficients, p-value and a description are returned.

Usage

1
batch.effects.lm.e(XP.conditions, XP.names, pathout, nvert=12)

Arguments

XP.conditions

Vector of experimental conditions for each sample

XP.names

Vector of names for each sample

pathout

Address where output files will be written

nvert

Number of legend items which can be displayed corectly, 12 by default

Value

This function returns a list containing the following :

plot

Address of png plot file

value

Minimum p-value obtained from the fits

color

Color white/orange/red corresponding to good/warning/poor level of quality

recommendation

Description and recommendation based on value

recommendation.mat

Matrix of coefficients for each fit

Examples

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# Sequenced reads aligned to mRNA (and containing no rRNA, depleted previously),
#   in bam format
readsBAM.1.1  <- paste(system.file(package="RiboVIEW", mustWork = TRUE), 
                                              "/extdata/Cond1-Rep1.bam",sep="")
readsBAM.1.2  <- paste(system.file(package="RiboVIEW", mustWork = TRUE), 
                                              "/extdata/Cond1-Rep2.bam",sep="")
readsBAM.1.3  <- paste(system.file(package="RiboVIEW", mustWork = TRUE), 
                                              "/extdata/Cond1-Rep3.bam",sep="")
readsBAM.2.1  <- paste(system.file(package="RiboVIEW", mustWork = TRUE), 
                                              "/extdata/Cond2-Rep1.bam",sep="")
readsBAM.2.2  <- paste(system.file(package="RiboVIEW", mustWork = TRUE), 
                                              "/extdata/Cond2-Rep2.bam",sep="")
readsBAM.2.3  <- paste(system.file(package="RiboVIEW", mustWork = TRUE), 
                                              "/extdata/Cond2-Rep3.bam",sep="")

list.bam <- list(readsBAM.1.1, readsBAM.1.2, readsBAM.1.3, 
                 readsBAM.2.1, readsBAM.2.2, readsBAM.2.3)


#
## Experimental conditions, in text and as indicators :
#    0 for control
#    1 for a condition, treatment, case, etc...
#    2, 3, etc. for further conditions

XP.conditions   <- c("cond1","cond1","cond1","cond2", "cond2","cond2")
XP.conditions.i <- c( 1,1,1,2,2,2)
XP.names        <- c("C1.R1", "C1.R2", "C1.R3", 
                     "C2.R1", "C2.R2", "C2.R3")

#
## Reference annotation for mRNAs' CDS.
#

refCDS <- paste(system.file(package="RiboVIEW", mustWork = TRUE), "/extdata/synth.tsv", sep="")
# Note : CDS annotation can be obtained from a GTF file, 
#        using gtf2table(my-gtf-file, outfile = my-cds-file)
#        (for example GTF file as provided by Ensembl.org work well with gtf2table)

#
## Reference sequences for mRNAs.
#

refFASTA <- paste(system.file(package="RiboVIEW", mustWork = TRUE), "/extdata/synth.fasta", sep="")

#
## Work and output folder.
#

pathout  <-  paste(tempdir(),"/", sep="")
  ## !! This is a temporary directory, which will be erased when you leave R !!
  ##   For your own analyses you would probably prefer to point to a permanent repository :
  #      pathout <- /home/me/address-to-my-output-repository/ # Define address, 
  #                                                   #including a final slash.
  #      system(paste('mkdir',pathout)) # Create folder at said address.
  #      setwd(pathout)  # Go to this directory. This is useful if you want to 
  #                                         #save additional tables or figures.

# 
## A-site coverage periodicity by length
#

periodicity(list.bam, refCDS, refFASTA, pathout, XP.names, versionStrip = FALSE)

# 
## Select footprint length with sufficient periodicity
#

attach(listminmax <- select.FPlen(list.bam, pathout, XP.names))

#
## Codon occupancy, codon enrichment.
# 

enrichmentNoccupancy(list.bam, refCDS, refFASTA, mini, maxi, XP.names,  
                       pathout, versionStrip = FALSE)

#
## Batch effects
#

batch.effects.lm.e.res <- batch.effects.lm.e(XP.conditions, XP.names, pathout)
batch.effects.lm.e.res

batch.effects.pca.res <- batch.effects.pca(XP.conditions, XP.names, pathout)
batch.effects.pca.res

carinelegrand/RiboVIEW documentation built on July 17, 2020, 3:02 p.m.

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RiboVIEW: Visualization, Quality Control and Statistical Analysis for Ribosome Profiling data

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