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R/narrowpeaksDiff.R
In NarrowPeaks: Shape-based Analysis of Variation in ChIP-seq using Functional PCA
Defines functions
narrowpeaksDiff
Documented in
narrowpeaksDiff
narrowpeaksDiff <- function(bedFile, headerBed= TRUE, flank=100, bigwigs , conditions , nbasis=50, pcs = 10, bigWigSummaryPath=getwd(), variation = 0.6) {
# Read BED file (chr start end ref)
bed <- read.table(bedFile, header = headerBed);
if (dim(bed)[2] > 3){
bed <- bed[,1:4]
colnames(bed) <- c("chr", "start", "end", "ref")
bed$start <- bed$ref - flank
bed$end <- bed$ref + flank
}
if (dim(bed)[2] == 3){ # If only chr,start,end; then we take the midpoint as reference
bed <- bed[,1:3]
colnames(bed) <- c("chr", "start", "end")
ref <- round((bed$start + bed$end)/2)
bed$start <- ref - flank
bed$end <- ref + flank
}
fdamatrix <- list() #To store profiles of all datasets
for (k in 1:length(bigwigs) ){
fdamatrix[[k]] <- matrix(0.0,ncol=1+2*flank, nrow= length(bed$chr) )
for (i in 1:length(bed$chr)) {
#owd <- setwd(tempdir())
randString <- getRandString()
UCSC <- paste(bigWigSummaryPath,"/bigWigSummary", sep="")
cmmd <- paste(UCSC, bigwigs[k], bed$chr[i], as.integer(bed$start[i]), as.integer(bed$end[i]), as.integer(1+2*flank), paste("> temp",".txt",sep=randString), sep=' ')
x <- system(cmmd, intern=FALSE);
if(length(readLines(paste("temp",".txt",sep=randString )))>0) { #if no data the file is empty
#if(length(x)==1) {
x <- as.numeric( strsplit(x= readLines(paste("temp",".txt",sep=randString )) ,split="\t")[[1]])
fdamatrix[[k]][i,] <- x
#}
}
system(paste("rm",paste("temp",".txt",sep=randString) ,sep=' '), intern=FALSE);
rm(x,randString)
}
# here we have the matrix with all the profiles
# correct non-numeric values in case of NAs
fdamatrix[[k]][which(is.na(fdamatrix[[k]])==TRUE)] <- 0.0
fdamatrix[[k]][which(is.nan(fdamatrix[[k]])==TRUE)] <- 0.0
fdamatrix[[k]][which(is.numeric(fdamatrix[[k]])==FALSE)] <- 0.0
}
#List of matrices with the profile data ready#
#Create list of data.frames for the p-values
PVALS <- list()
uniqueCond <- unique(conditions)
for(j in 1:length(bed$chr) ){
Mtemp <- matrix(NA, ncol=length(uniqueCond), nrow=length(uniqueCond))
colnames(Mtemp) <- uniqueCond
rownames(Mtemp) <- uniqueCond
PVALS[[j]] <- as.data.frame(Mtemp)
rm(Mtemp)
}
#print(PVALS)
#FPCA:
bspl <- create.bspline.basis(rangeval=c(-flank,flank),nbasis=nbasis, norder=4)
argvalsBS <- -flank:flank
for(j in 1:length(bed$chr) ){
tempMatrix <- matrix(0.0, ncol=1+2*flank, nrow= length(bigwigs) )
for (m in 1:length(bigwigs)) {
tempMatrix[m,] <- fdamatrix[[m]][j,]
}
fdaData <- Data2fd(y=t(tempMatrix), argvals= argvalsBS, basisobj=bspl)
#plot.fd(fdaData)
pc <- pca.fd(fdobj=fdaData, nharm = pcs, harmfdPar=fdPar(fdaData),centerfns = TRUE)
#plot.fd(pc$harmonics)
# Select the PC scores for the components which amount >= 'variation'
#print(pc$varprop)
CS <- cumsum(pc$varprop)
requiredPCs <- which(CS >= variation)[1]
# Hotelling's T2 test between the conditions provided
for (o in 1:length(uniqueCond)){
for (p in 1:length(uniqueCond)){
Xid <- which(conditions == uniqueCond[o] )
Yid <- which(conditions == uniqueCond[p] )
PVALS[[j]][o,p] <- HotellingsT2(X=as.matrix(pc$scores[Xid ,1:requiredPCs],ncol=requiredPCs),Y=as.matrix(pc$scores[Yid,1:requiredPCs],ncol=requiredPCs), test="chi")$p.value
}
}
# report the P-values in a list of data.frames (PVALS)
}
return(list(fdaprofiles=fdamatrix, p.values = PVALS ) ) # report P-values!
}
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NarrowPeaks documentation built on April 28, 2020, 6:51 p.m.
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Defines functions narrowpeaksDiff
Documented in narrowpeaksDiff
narrowpeaksDiff <- function(bedFile, headerBed= TRUE, flank=100, bigwigs , conditions , nbasis=50, pcs = 10, bigWigSummaryPath=getwd(), variation = 0.6) {
# Read BED file (chr start end ref)
bed <- read.table(bedFile, header = headerBed);
if (dim(bed)[2] > 3){
bed <- bed[,1:4]
colnames(bed) <- c("chr", "start", "end", "ref")
bed$start <- bed$ref - flank
bed$end <- bed$ref + flank
}
if (dim(bed)[2] == 3){ # If only chr,start,end; then we take the midpoint as reference
bed <- bed[,1:3]
colnames(bed) <- c("chr", "start", "end")
ref <- round((bed$start + bed$end)/2)
bed$start <- ref - flank
bed$end <- ref + flank
}
fdamatrix <- list() #To store profiles of all datasets
for (k in 1:length(bigwigs) ){
fdamatrix[[k]] <- matrix(0.0,ncol=1+2*flank, nrow= length(bed$chr) )
for (i in 1:length(bed$chr)) {
#owd <- setwd(tempdir())
randString <- getRandString()
UCSC <- paste(bigWigSummaryPath,"/bigWigSummary", sep="")
cmmd <- paste(UCSC, bigwigs[k], bed$chr[i], as.integer(bed$start[i]), as.integer(bed$end[i]), as.integer(1+2*flank), paste("> temp",".txt",sep=randString), sep=' ')
x <- system(cmmd, intern=FALSE);
if(length(readLines(paste("temp",".txt",sep=randString )))>0) { #if no data the file is empty
#if(length(x)==1) {
x <- as.numeric( strsplit(x= readLines(paste("temp",".txt",sep=randString )) ,split="\t")[[1]])
fdamatrix[[k]][i,] <- x
#}
}
system(paste("rm",paste("temp",".txt",sep=randString) ,sep=' '), intern=FALSE);
rm(x,randString)
}
# here we have the matrix with all the profiles
# correct non-numeric values in case of NAs
fdamatrix[[k]][which(is.na(fdamatrix[[k]])==TRUE)] <- 0.0
fdamatrix[[k]][which(is.nan(fdamatrix[[k]])==TRUE)] <- 0.0
fdamatrix[[k]][which(is.numeric(fdamatrix[[k]])==FALSE)] <- 0.0
}
#List of matrices with the profile data ready#
#Create list of data.frames for the p-values
PVALS <- list()
uniqueCond <- unique(conditions)
for(j in 1:length(bed$chr) ){
Mtemp <- matrix(NA, ncol=length(uniqueCond), nrow=length(uniqueCond))
colnames(Mtemp) <- uniqueCond
rownames(Mtemp) <- uniqueCond
PVALS[[j]] <- as.data.frame(Mtemp)
rm(Mtemp)
}
#print(PVALS)
#FPCA:
bspl <- create.bspline.basis(rangeval=c(-flank,flank),nbasis=nbasis, norder=4)
argvalsBS <- -flank:flank
for(j in 1:length(bed$chr) ){
tempMatrix <- matrix(0.0, ncol=1+2*flank, nrow= length(bigwigs) )
for (m in 1:length(bigwigs)) {
tempMatrix[m,] <- fdamatrix[[m]][j,]
}
fdaData <- Data2fd(y=t(tempMatrix), argvals= argvalsBS, basisobj=bspl)
#plot.fd(fdaData)
pc <- pca.fd(fdobj=fdaData, nharm = pcs, harmfdPar=fdPar(fdaData),centerfns = TRUE)
#plot.fd(pc$harmonics)
# Select the PC scores for the components which amount >= 'variation'
#print(pc$varprop)
CS <- cumsum(pc$varprop)
requiredPCs <- which(CS >= variation)[1]
# Hotelling's T2 test between the conditions provided
for (o in 1:length(uniqueCond)){
for (p in 1:length(uniqueCond)){
Xid <- which(conditions == uniqueCond[o] )
Yid <- which(conditions == uniqueCond[p] )
PVALS[[j]][o,p] <- HotellingsT2(X=as.matrix(pc$scores[Xid ,1:requiredPCs],ncol=requiredPCs),Y=as.matrix(pc$scores[Yid,1:requiredPCs],ncol=requiredPCs), test="chi")$p.value
}
}
# report the P-values in a list of data.frames (PVALS)
}
return(list(fdaprofiles=fdamatrix, p.values = PVALS ) ) # report P-values!
}
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