Description Usage Arguments Details Value Note Author(s) See Also Examples
Compute the RIPScore using only the RIP (typically when control is unavailable) posteriors for each bins, merge and summarize the scores for the merged bins, and finally compute the p-value and adjusted p-value for the summary RIPScore.
1 | logScoreWithoutControl(nbhGRRIP, padjMethod = "BH")
|
nbhGRRIP |
GRanges object for the RIP library created from |
padjMethod |
Method used to adjust multiple testing performed in |
The RIPScore is compupted in computeLogOdd
as the log odd ratio of the posterior for the RIP state (z_{i} = 2) over the posterior for the background state (z_{i} = 1) in RIP library alone (typically when control is unavailable). The adjacent bins with hidden states predicted by nbh_vit
as the enriched state (corresponding to the NB with larger mean) are merged. The RIPSscores are averaged over the merged bins. To assess the statistical significance of the RIPScore for each region, we assume that the RIPScore follows a Gaussian (Normal) distribution with mean and standard deviation estimated using the RIPScores over all of the bins. The rationale is based on the assumption that most of the RIPScores correspond to the background state and together contribute to a stable estimate of the test statistics (TS) and p-value computed using the R built-in function pnorm
. The p-value is adjusted by p.adjust
with BH method by default.
GRanges
of merged bins with values slot saved for RIPScore (lodOdd), p-value (pval), adjusted p-value (pvalAdj) for RIP
Internal function used by seekRIP
.
Yue Li
logScoreWithControl, seekRIP, computeLogOdd, scoreMergedBins
1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 19 20 21 22 23 24 25 26 | if(interactive()) { # check the example in seekRIP
# Retrieve system files
extdata.dir <- system.file("extdata", package="RIPSeeker")
bamFiles <- list.files(extdata.dir, ".bam$", recursive=TRUE, full.names=TRUE)
bamFiles <- grep("PRC2", bamFiles, value=TRUE)
# Parameters setting
binSize <- 1e5 # use a large fixed bin size for demo only
multicore <- FALSE # use multicore
strandType <- "-" # set strand type to minus strand
################ run main function for HMM inference on all chromosomes ################
mainSeekOutputRIP <- mainSeek(bamFiles=grep(pattern="SRR039214",
bamFiles, value=TRUE, invert=TRUE),
binSize=binSize, strandType=strandType,
reverseComplement=TRUE, genomeBuild="mm9",
uniqueHit = TRUE, assignMultihits = TRUE,
rerunWithDisambiguatedMultihits = FALSE,
multicore=multicore, silentMain=FALSE, verbose=TRUE)
################ Compute log score and test for significance WITHOUT control ################
ripGR.wocontrol <- logScoreWithoutControl(mainSeekOutputRIP$nbhGRList$chrX)
}
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