R/methods-CNSet.R
In crlmm: Genotype Calling (CRLMM) and Copy Number Analysis tool for Affymetrix SNP 5.0 and 6.0 and Illumina arrays

setMethod("posteriorMean", signature(object="CNSet"), function(object) assayDataElement(object, "posteriorMean"))
setReplaceMethod("posteriorMean", signature(object="CNSet", value="matrix"), function(object, value) assayDataElementReplace(object, "posteriorMean", value))
##setReplaceMethod("mixtureParams", signature(object="CNSet", value="ANY"), function(object, value) object@mixtureParams <- mixtureParams)

linearParamElementReplace <- function(obj, elt, value) {
    storage.mode <- storageMode(batchStatistics(obj))
    switch(storage.mode,
           "lockedEnvironment" = {
               aData <- copyEnv(batchStatistics(obj))
               if (is.null(value)) rm(list=elt, envir=aData)
               else aData[[elt]] <- value
               Biobase:::assayDataEnvLock(aData)
               batchStatistics(obj) <- aData
           },
           "environment" = {
               if (is.null(value)) rm(list=elt, envir=batchStatistics(obj))
               else batchStatistics(obj)[[elt]] <- value
           },
           list = batchStatistics(obj)[[elt]] <- value)
    obj
}

## parameters
## allele A
##   autosome SNPs
##   autosome NPs
##   chromosome X NPs for women
C1 <- function(object, marker.index, batch.index, sample.index){
	acn <- matrix(NA, nrow=length(marker.index), ncol=length(sample.index))
	for(k in seq_along(batch.index)){
		l <- batch.index[k]
		## calculate cn for all the samples that are in this batch
		jj <- sample.index[as.character(batch(object))[sample.index] == batchNames(object)[l]]
		bg <- nuA(object)[marker.index, l]
		slope <- phiA(object)[marker.index, l]
		I <- as.matrix(A(object)[marker.index, jj])
		acn[, match(jj, sample.index)] <- 1/slope * (I - bg)
	}
	return(as.matrix(acn))
}

## allele B  (treated allele 'A' for chromosome X NPs)
##   autosome SNPs
##   chromosome X for male nonpolymorphic markers
C2 <- function(object, marker.index, batch.index, sample.index, NP.X=FALSE){
	acn <- matrix(NA, nrow=length(marker.index), ncol=length(sample.index))
	for(k in seq_along(batch.index)){
		l <- batch.index[k]
		jj <- sample.index[as.character(batch(object))[sample.index] == batchNames(object)[l]]
		bg <- nuB(object)[marker.index, l]
		slope <- phiB(object)[marker.index, l]
		if(!NP.X){
			I <- as.matrix(B(object)[marker.index, jj])
		} else I <- as.matrix(A(object)[marker.index, jj])
		acn[, match(jj, sample.index)] <- 1/slope * (I - bg)
	}
##	if(length(acn) > 1){
##		acn <- do.call("cbind", acn)
##	} else acn <- acn[[1]]
	return(as.matrix(acn))
}

## Chromosome X SNPs
C3 <- function(object, allele, marker.index, batch.index, sample.index){
##	acn <- vector("list", length(batch.index))
	acn <- matrix(NA, nrow=length(marker.index), ncol=length(sample.index))
	for(k in seq_along(batch.index)){
		l <- batch.index[k]
		##j <- which(as.character(batch(object))[sample.index] == batchNames(object)[l])
		jj <- sample.index[as.character(batch(object))[sample.index] == batchNames(object)[l]]
		##phiA2 and phiB2 are not always estimable  -- need both men and women
		phiA2 <- phiPrimeA(object)[marker.index, l]
		phiB2 <- phiPrimeB(object)[marker.index, l]
		phiA <- phiA(object)[marker.index, l]
		phiB <- phiB(object)[marker.index, l]
		nuA <- nuA(object)[marker.index, l]
		nuB <- nuB(object)[marker.index, l]
		phiA <- phiA(object)[marker.index, l]
		IA <- as.matrix(A(object)[marker.index, jj])
		IB <- as.matrix(B(object)[marker.index, jj])
		## I = nu + acn * phi
		## acn = 1/phi* (I-nu)
		phistar <- phiB2/phiA
		tmp <- (IB - nuB - phistar*IA + phistar*nuA)/phiB
		CB <- tmp/(1-phistar*phiA2/phiB)
		index <- which(is.na(phiB2) | is.na(phiA2))
		if(length(index) > 0){
			cb <- 1/phiB[index] * (IB[index, ] - nuB[index])
			CB[index, ] <- cb
		}
		if(allele == "B"){
			acn[, match(jj, sample.index)] <- CB
			##acn[[k]] <- CB
		}
		if(allele == "A"){
			CA <- (IA-nuA-phiA2*CB)/phiA
			if(length(index) > 0){
				ca <- 1/phiA[index] * (IA[index, ] - nuA[index])
 				CA[index, ] <- ca
			}
			acn[, match(jj, sample.index)] <- CA
		}
	}
##	if(length(acn) > 1){
##		acn <- do.call("cbind", acn)
##	} else acn <- acn[[1]]
	return(as.matrix(acn))
}




ACN <- function(object, allele, i , j){
	if(missing(i) & missing(j)) stop("must specify rows (i) or columns (j)")
	is.ff <- is(calls(object), "ff") | is(calls(object), "ffdf")
	missing.i <- missing(i)
	missing.j <- missing(j)
	if(!missing.i){
		is.ann <- !is.na(chromosome(object)[i])
		is.X <- chromosome(object)[i]==23 & is.ann
		is.auto <- chromosome(object)[i] < 23 & is.ann
		is.snp <- isSnp(object)[i] & is.ann
	} else{
		is.ann <- !is.na(chromosome(object))
		is.X <- chromosome(object)==23 & is.ann
		is.auto <- chromosome(object) < 23 & is.ann
		is.snp <- isSnp(object) & is.ann
		i <- 1:nrow(object)
	}
	## Define batch.index and sample.index
	if(!missing.j) {
		batches <- unique(as.character(batch(object)[j]))
		##batches <- as.character(batch(object)[j])
		batch.index <- match(batches, batchNames(object))
	} else {
		batch.index <- seq_along(batchNames(object))
		j <- 1:ncol(object)
	}
	nr <- length(i)
	nc <- length(j)
	acn <- matrix(NA, nr, nc)
	dimnames(acn) <- list(featureNames(object)[i],
			      sampleNames(object)[j])
	if(allele == "A"){
		if(is.ff){
			open(nuA(object))
			open(phiA(object))
			open(A(object))
		}
		## --
		## 4 types of markers for allele A
		##--
		## 1. autosomal SNPs or autosomal NPs
		if(any(is.auto)){
			auto.index <- which(is.auto)
			marker.index <- i[is.auto]
			acn[auto.index, ] <- C1(object, marker.index, batch.index, j)
		}
		if(any(is.X)){
			##2. CHR X SNPs (men and women)
			if(any(is.snp)){
				if(is.ff) {
					open(phiPrimeA(object))
					open(phiPrimeB(object))
					open(phiB(object))
					open(nuB(object))
					open(B(object))
				}
				marker.index <- i[is.X & is.snp]
				acn.index <- which(is.X & is.snp)
				acn[acn.index, ] <- C3(object, allele="A", marker.index, batch.index, j)
				if(is.ff) {
					close(phiPrimeA(object))
					close(phiPrimeB(object))
					close(phiB(object))
					close(nuB(object))
					close(B(object))
				}
			}
			if(any(!is.snp)){
				marker.index <- i[is.X & !is.snp]
				acn.index <- which(is.X & !is.snp)
				acn[acn.index, ] <- NA
				female.index <- j[object$gender[j] == 2]
				## 3. CHR X NPs: women
				if(length(female.index) > 0){
					female.batch.index <- match(unique(as.character(batch(object))[female.index]), batchNames(object))
					jj <- which(object$gender[j] == 2)
					acn[acn.index, jj] <- C1(object, marker.index, female.batch.index, female.index)
				}
				male.index <- j[object$gender[j] == 1]
				if(length(male.index) > 0){
					if(is.ff){
						open(nuB(object))
						open(phiB(object))
					}
					male.batch.index <- match(unique(as.character(batch(object))[male.index]), batchNames(object))
					jj <- which(object$gender[j] == 1)
					acn[acn.index, jj] <- C2(object, marker.index, male.batch.index, male.index, NP.X=TRUE)
					if(is.ff){
						close(nuB(object))
						close(phiB(object))
					}
				}
			}
		}
		if(is.ff){
			close(nuA(object))
			close(phiA(object))
			close(A(object))
		}
	}
	if(allele == "B"){
		if(is.ff){
			open(nuB(object))
			open(phiB(object))
			open(B(object))
		}
		if(any(!is.snp)){
			acn.index <- which(!is.snp)
			acn[acn.index, ] <- 0
		}
		if(any(is.auto)){
			auto.index <- which(is.auto & is.snp)
			if(length(auto.index) > 0){
				marker.index <- i[auto.index]
				acn[auto.index, ] <- C2(object, marker.index, batch.index, j)
			}
		}
		if(any(is.X)){
			if(is.ff){
				open(phiPrimeA(object))
				open(phiPrimeB(object))
				open(phiA(object))
				open(nuA(object))
				open(A(object))
			}
			marker.index <- i[is.X & is.snp]
			acn.index <- which(is.X & is.snp)
			acn[acn.index, ] <- C3(object, allele="B", marker.index, batch.index, j)
			if(is.ff){
				close(phiPrimeA(object))
				close(phiPrimeB(object))
				close(phiA(object))
				close(nuA(object))
				close(A(object))
			}
			if(any(!is.snp)){
				acn.index <- which(!is.snp)
				marker.index <- i[!is.snp]
				acn[acn.index, ] <- 0
			}
		}
	}
	if(is.ff){
		close(nuB(object))
		close(phiB(object))
		close(B(object))
	}
	return(acn)
}

setMethod("CA", signature=signature(object="CNSet"),
	  function(object, ...){
		  ca <- ACN(object, allele="A", ...)
		  ca[ca < 0] <- 0
		  ca[ca > 5] <- 5
		  return(ca)
	  })
setMethod("CB", signature=signature(object="CNSet"),
	  function(object, ...) {
		  cb <- ACN(object, allele="B", ...)
		  cb[cb < 0] <- 0
		  cb[cb > 5] <- 5
		  return(cb)
	  })

setMethod("totalCopynumber", signature=signature(object="CNSet"),
	  function(object, ...){
		  ca <- CA(object, ...)
		  cb <- CB(object, ...)
		  return(ca+cb)
	  })
rawCopynumber <- totalCopynumber

setMethod("posteriorProbability", signature(object="CNSet"),
	  function(object, predictRegion, copyNumber=0:4, w){
		  if(missing(w)) w <- rep(1/length(copyNumber),length(copyNumber))
		  stopifnot(sum(w)==1)
		  logI <- array(NA, dim=c(nrow(object), ncol(object), 2), dimnames=list(NULL, NULL, LETTERS[1:2]))
		  getIntensity <- function(object){
			  logI[, , 1] <- log2(A(object))
			  logI[, , 2] <- log2(B(object))
			  return(logI)
		  }
		  logI <- getIntensity(object)
		  ##gts <- lapply(as.list(0:4), genotypes)
		  prob <- array(NA, dim=c(nrow(object), ncol(object), length(copyNumber)),
				dimnames=list(NULL,NULL, paste("copynumber",copyNumber, sep="")))
		  bns <- batchNames(object)
		  snp.index <- which(isSnp(object))
		  if(length(snp.index) > 0){
			  for(i in seq_along(copyNumber)){
				  G <- genotypes(copyNumber[i])
				  P <- array(NA, dim=c(length(snp.index), ncol(object), length(G)),
					     dimnames=list(NULL,NULL,G))
				  for(g in seq_along(G)){
					  gt <- G[g]
					  for(j in seq_along(bns)){
						  this.batch <- bns[j]
						  sample.index <- which(batch(object) == this.batch)
						  mu <- predictRegion[[gt]]$mu[snp.index, , this.batch, drop=FALSE]
						  dim(mu) <- dim(mu)[1:2]
						  if(all(is.na(mu))){
							  P[, sample.index, gt] <- NA
						  } else {
							  Sigma <- predictRegion[[gt]]$cov[snp.index, , this.batch, drop=FALSE]
							  dim(Sigma) <- dim(Sigma)[1:2]
							  P[, sample.index, gt] <- dbvn(x=logI[snp.index, sample.index, , drop=FALSE], mu=mu, Sigma=Sigma)
						  }
					  }
				  }
				  ## the marginal probability for the total copy number
				  ##  -- integrate out the probability for the different genotypes
				  for(j in 1:ncol(P)){
					  PP <- P[, j, , drop=FALSE]
					  dim(PP) <- dim(PP)[c(1, 3)]
					  prob[snp.index, j, i] <- rowSums(PP, na.rm=TRUE)
				  }
			  }
		  } ## length(snp.index) > 0
		  ##---------------------------------------------------------------------------
		  ##
		  ##  nonpolymorphic markers
		  ##
		  ##---------------------------------------------------------------------------
		  np.index <- which(!isSnp(object))
		  if(length(np.index) > 0){
			  for(i in seq_along(copyNumber)){
				  G <- genotypes(copyNumber[i], is.snp=FALSE)
				  P <- array(NA, dim=c(length(np.index), ncol(object), length(G)),
					     dimnames=list(NULL,NULL,G))
				  for(g in seq_along(G)){
					  gt <- G[g]
					  for(j in seq_along(bns)){
						  this.batch <- bns[j]
						  sample.index <- which(batch(object) == this.batch)
						  mu <- predictRegion[[gt]]$mu[np.index, 1, this.batch, drop=FALSE]
						  dim(mu) <- dim(mu)[1]
						  if(all(is.na(mu))){
							  P[, sample.index, gt] <- NA
						  } else {
							  Sigma <- predictRegion[[gt]]$cov[np.index, 1, this.batch, drop=FALSE]
							  dim(Sigma) <- dim(Sigma)[1]
							  P[, sample.index, gt] <- dnorm(logI[np.index, sample.index, 1], mean=mu, sd=Sigma)
						  }
					  } ## j in seq_along(bns)
				  } ## g in seq_along(G)
				  ## the marginal probability for the total copy number
				  ##  -- integrate out the probability for the different genotypes
				  prob[np.index, , i] <- P
			  } ## seq_along(copyNumber)
		  } ## length(np.index) > 0
		  ##constant.  Probs across copy number states must
		  ##sum to one.  nc <- apply(prob, c(1,3), sum,
		  ##na.rm=TRUE)
		  wm <- matrix(w, nrow(object), length(copyNumber), byrow=TRUE)
		  nc <- matrix(NA, nrow(object), ncol(object))
		  for(j in seq_len(ncol(object))){
			  pp <- prob[, j, ] * wm
			  nc <- rowSums(pp, na.rm=TRUE)
			  prob[, j, ] <- pp/nc
		  }
		  return(prob)
	  })

setMethod("calculatePosteriorMean", signature(object="CNSet"),
	  function(object, posteriorProb, copyNumber=0:4, ...){
		  stopifnot(dim(posteriorProb)[[3]] == length(copyNumber))
		  pm <- matrix(0, nrow(object), ncol(object))
		  for(i in seq_along(copyNumber)){
			  pm <- pm + posteriorProb[, , i] * copyNumber[i]
		  }
		  return(pm)
	  })

##.bivariateCenter <- function(nu, phi){
##			  ##  lexical scope for mus, CA, CB
##			  if(CA <= 2 & CB <= 2 & (CA+CB) < 4){
##				  mus[,1, ] <- log2(nu[, 1, ] + CA *
##						    phi[, 1, ])
##				  mus[,2, ] <- log2(nu[, 2, ] + CB *
##						    phi[, 2, ])
##			  } else { ## CA > 2
##				  if(CA > 2){
##					  theta <- pi/4*Sigma[,2,]
##					  shiftA <- CA/4*phi[, 1, ] * cos(theta)
##					  shiftB <- CA/4*phi[, 1, ] * sin(theta)
##					  mus[, 1, ] <- log2(nu[, 1, ] + 2 * phi[,1,]+shiftA)
##					  mus[, 2, ] <- log2(nu[, 2, ] + CB *phi[,2,]+shiftB)
##				  }
##				  if(CB > 2){
##					  ## CB > 2
##					  theta <- pi/2-pi/4*Sigma[,2,]
##					  shiftA <- CB/4*phi[, 2, ] * cos(theta)
##					  shiftB <- CB/4*phi[, 2, ] * sin(theta)
##					  mus[, 1, ] <- log2(nu[, 1, ] + CA*phi[,1,]+shiftA)
##					  mus[, 2, ] <- log2(nu[, 2, ]+ 2*phi[,2,]+shiftB)
##				  }
##				  if(CA == 2 & CB == 2){
##					  mus[, 1, ] <- log2(nu[, 1, ] + 1/2*CA*phi[,1,])
##					  mus[, 2, ] <- log2(nu[, 2, ]+ 1/2*CB*phi[,2,])
##				  }
##			  }
##			  mus
##		  }

## for a given copy number, return a named list of bivariate normal prediction regions
##   - elements of list are named by genotype
##   'AAA'  list should have 'mu' and 'Sigma'
##                mu is a R x 2 matrix, R is number of features
##                Sigma is a R x 4 matrix.  Each row can be coerced to a 2 x 2 matrix
##          For nonpolymorphic markers, 2nd column of mu is NA and elements 2-4 of Sigma are NA
##
setMethod("predictionRegion", signature(object="CNSet", copyNumber="integer"),
	  function(object, copyNumber=0:4){
		  ## would it be more efficient to store as an array?
		  ## mu: features x genotype x allele
		  ## Sigma: features x genotype x covariance
		  stopifnot(all(copyNumber %in% 0:4))
		  getNu <- function(object){
			  nu[, 1, ] <- nuA(object)
			  nu[, 2, ] <- nuB(object)
			  nu
		  }
		  getPhi <- function(object){
			  phi[,1,] <- phiA(object)
			  phi[,2,] <- phiB(object)
			  phi
		  }
		  gts <- lapply(as.list(copyNumber), genotypes)
		  nms <- unlist(gts)
		  res <- vector("list", length(nms))
		  ##names(res) <- paste("copyNumber", copyNumber, sep="")
		  names(res) <- nms
		  bnms <- batchNames(object)
		  nu <- array(NA, dim=c(nrow(object), 2, length(bnms)))
		  phi <- array(NA, dim=c(nrow(object), 2, length(bnms)))
		  nu <- getNu(object)
		  phi <- getPhi(object)
		  ##mus <- matrix(NA, nrow(nu), 2, dimnames=list(NULL, LETTERS[1:2]))
		  mus <- array(NA, dim=c(nrow(nu), 2, length(bnms)),
			       dimnames=list(NULL, LETTERS[1:2],
			       bnms))
		  ## Sigma <- matrix(NA, nrow(nu), 3)
		  Sigma <- array(NA, dim=c(nrow(nu), 3, length(bnms)),
				 dimnames=list(NULL, c("varA", "cor", "varB"),
				 bnms))
		  bivariateCenter <- function(nu, phi){
			  ##  lexical scope for mus, CA, CB
			  mus[,1, ] <- log2(nu[, 1, ] + CA *
					    phi[, 1, ])
			  mus[,2, ] <- log2(nu[, 2, ] + CB *
					    phi[, 2, ])
			  return(mus)
		  }
		  np.index <- which(!isSnp(object))
		  for(i in seq_along(copyNumber)){
			  G <- genotypes(copyNumber[i])
			  tmp <- vector("list", length(G))
			  names(tmp) <- G
			  CN <- copyNumber[i]
			  for(g in seq_along(G)){
				  gt <- G[g]
				  CB <- g-1
				  CA <- CN-CB
				  gt.corr <- genotypeCorrelation(gt)
				  nma <- ifelse(CA == 0, "tau2A.BB", "tau2A.AA")
				  nmb <- ifelse(CB == 0, "tau2B.AA", "tau2B.BB")
				  Sigma[, 1, ] <- getVar(object, nma)
				  Sigma[, 3, ] <- getVar(object, nmb)
				  Sigma[, 2, ] <- getCor(object, gt.corr)
				  if(length(np.index) > 0){
					  Sigma[, 1, ] <- getVar(object, "tau2A.AA")
					  Sigma[np.index, 2, ] <- NA
				  }
				  res[[gt]]$mu <- bivariateCenter(nu,phi)
				  ## adjust correlation
##				  if(CA == 0 | CB == 0){
##					  Sigma[,2,] <- 0
##				  }
				  res[[gt]]$cov <- Sigma
			  }
		  }
		  res <- as(res, "PredictionRegion")
		  return(res)
	  })



setMethod("xyplotcrlmm", signature(x="formula", data="CNSet", predictRegion="list"),
	  function(x, data, predictRegion, ...){
		  fns <- featureNames(data)
		  fns <- matrix(fns, nrow(data), ncol(data), byrow=FALSE)
		  fns <- as.character(fns)
		  df <- list(A=as.numeric(log2(A(data))),
			     B=as.numeric(log2(B(data))),
			     gt=as.integer(calls(data)),
			     gt.conf=as.numeric(confs(data)),
			     snpid=fns)#, snp=snpId)
		  df <- as.data.frame(df)
		  df$snpid <- factor(df$snpid, levels=unique(df$snpid), ordered=TRUE)
		  bns <- batchNames(data)
		  predictRegion <- lapply(predictRegion, function(x, bns){
			  batch.index <- match(bns, dimnames(x$mu)[[3]])
			  x$mu <- x$mu[, , batch.index, drop=FALSE]
			  x$cov <- x$cov[, , batch.index, drop=FALSE]
			  return(x)
		  }, bns=bns)
		  ##predictRegion is an argument of ABpanel
		  xyplot(x, df, predictRegion=predictRegion, ...)
	  })

setMethod("xyplot", signature(x="formula", data="CNSet"),
	  function(x, data, ...){
		  if("predictRegion" %in% names(list(...))){
			  xyplotcrlmm(x, data, ...)
		  } else{
			  callNextMethod()
		  }
})

setMethod("calculateRBaf", signature(object="CNSet"),
	  function(object, batch.name, chrom){
		  calculateRBafCNSet(object, batch.name, chrom)
	  })

calculateRBafCNSet <- function(object, batch.name, chrom){
	if(missing(batch.name)) {
		batch.name <- batchNames(object)
		if("grandMean" %in% batch.name)
			batch.name <- batch.name[-length(batch.name)]
	}
	if(missing(chrom)) chrom <- unique(chromosome(object))
	if(!(all(batch.name %in% batchNames(object)))) stop("batch.name must be belong to batchNames(object)")
	chr <- chromosome(object)
	valid.chrs <- chr <= 23 & chr %in% chrom
	index <- which(valid.chrs)
	indexlist <- split(index, chr[index])
	J <- which(batch(object) %in% batch.name)
	sns <- sampleNames(object)[J]
	sampleindex <- split(J, factor(batch(object)[J], levels=unique(batch(object)[J])))
	if(!all(valid.chrs)) warning("Only computing log R ratios and BAFs for autosomes and chr X")
	## if ff package is loaded, these will be ff objects
	chr <- names(indexlist)
	rlist <- blist <- vector("list", length(indexlist))
	path <- ldPath()
	processByChromosome <- function(i, chr, path){
		ldPath(path)
		nr <- length(i)
		##CHR <- names(i)
		bafname <- paste("baf_chr", chr, sep="")
		rname <- paste("lrr_chr", chr, sep="")
		bmatrix <- initializeBigMatrix(bafname, nr=nr, nc=length(sns), vmode="integer")
		rmatrix <- initializeBigMatrix(rname, nr=nr, nc=length(sns), vmode="integer")
		colnames(rmatrix) <- colnames(bmatrix) <- sns
		## put rownames in order of physical position
		ix <- order(position(object)[i])
		i <- i[ix]
		rownames(rmatrix) <- rownames(bmatrix) <- featureNames(object)[i]
		for(j in seq_along(sampleindex)){
			bname <- batch.name[j]
			J <- sampleindex[[j]]
			res <- calculateRTheta(object=object, # crlmm:::
						       batch.name=bname,
						       feature.index=i)
			k <- match(sampleNames(object)[J], sns)
			bmatrix[, k] <- res[["baf"]]
			rmatrix[, k] <- res[["lrr"]]
		}
		list(bmatrix, rmatrix)
	}
	## calcualte R BAF by chromosome
	if(isPackageLoaded("ff")){
		pkgs <- c("oligoClasses", "ff", "Biobase", "crlmm")
	} else pkgs <- c("oligoClasses", "Biobase", "crlmm")
	i <- NULL
	res <- foreach(i=indexlist, chr=names(indexlist), .packages=pkgs) %dopar% {
		processByChromosome(i, chr, path)
	}
	blist <- lapply(res, "[[", 1)
	rlist <- lapply(res, "[[", 2)
	res <- list(baf=blist, lrr=rlist)
	return(res)
}

##setMethod("calculateRBaf", signature(object="CNSet"),
##	  function(object, batch.name){
##		  all.autosomes <- all(chromosome(object) < 23)
##		  if(!all.autosomes){
##			  stop("method currently only defined for chromosomes 1-22")
##		  }
##		  if(missing(batch.name)) batch.name <- batchNames(object)[1]
##		  stopifnot(batch.name %in% batchNames(object))
##		  if(length(batch.name) > 1){
##			  warning("only the first batch in batch.name processed")
##			  batch.name <- batch.name[1]
##		  }
##		  RTheta.aa <- calculateRTheta(object, "AA", batch.name)
##		  RTheta.ab <- calculateRTheta(object, "AB", batch.name)
##		  RTheta.bb <- calculateRTheta(object, "BB", batch.name)
##
##		  J <- which(batch(object) == batch.name)
##
##		  theta.aa <- matrix(RTheta.aa[, "theta"], nrow(object), length(J), byrow=FALSE)
##		  theta.ab <- matrix(RTheta.ab[, "theta"], nrow(object), length(J), byrow=FALSE)
##		  theta.bb <- matrix(RTheta.bb[, "theta"], nrow(object), length(J), byrow=FALSE)
##
##		  a <- A(object)[, J, drop=FALSE]
##		  b <- B(object)[, J, drop=FALSE] ## NA's for b where nonpolymorphic
##		  is.np <- !isSnp(object)
##		  ##b[is.np, ] <- a[is.np, ]
##		  b[is.np, ] <- 0L
##		  dns <- dimnames(a)
##		  dimnames(a) <- dimnames(b) <- NULL
##		  obs.theta <- atan2(b, a)*2/pi
##
##		  lessAA <- obs.theta < theta.aa
##		  lessAB <- obs.theta < theta.ab
##		  lessBB <- obs.theta < theta.bb
##		  grAA <- !lessAA
##		  grAB <- !lessAB
##		  grBB <- !lessBB
##		  not.na <- !is.na(theta.aa)
##		  I1 <- grAA & lessAB & not.na
##		  I2 <- grAB & lessBB & not.na
##
##		  bf <- matrix(NA, nrow(object), ncol(a))
##		  bf[I1] <- 0.5 * ((obs.theta-theta.aa)/(theta.ab-theta.aa))[I1]
##		  bf[I2] <- (.5 * (obs.theta - theta.ab) / (theta.bb - theta.ab))[I2] + 0.5
##		  bf[lessAA] <- 0
##		  bf[grBB] <- 1
##
##		  r.expected <- matrix(NA, nrow(object), ncol(a))
##		  r.aa <- matrix(RTheta.aa[, "R"], nrow(object), length(J), byrow=FALSE)
##		  r.ab <- matrix(RTheta.ab[, "R"], nrow(object), length(J), byrow=FALSE)
##		  r.bb <- matrix(RTheta.bb[, "R"], nrow(object), length(J), byrow=FALSE)
##		  rm(RTheta.aa, RTheta.ab, RTheta.bb); gc()
##		  obs.r <- a+b
##
##		  lessAA <- lessAA & not.na
##		  grBB <- grBB & not.na
##		  tmp <- ((obs.theta - theta.aa) * (r.ab-r.aa)/(theta.ab-theta.aa))[I1] + r.aa[I1]
##		  r.expected[I1] <- tmp
##		  tmp <- ((obs.theta - theta.ab) * (r.bb - r.ab)/(theta.bb-theta.ab))[I2] + r.ab[I2]
##		  r.expected[I2] <- tmp
##		  r.expected[lessAA] <- r.aa[lessAA]
##		  r.expected[grBB] <- r.bb[grBB]
##		  index.np <- which(is.np)
##		  if(length(index.np) > 0){
##			  a.np <- A(object)[index.np, J, drop=FALSE]
##			  meds <- rowMedians(a.np, na.rm=TRUE)
##			  r.expected[index.np, ] <- matrix(meds, length(index.np), ncol(a.np))
##		  }
##		  lrr <- log2(obs.r/r.expected)
##
##		  dimnames(bf) <- dimnames(lrr) <- dns
##		  res <- list(baf=bf,
##			      lrr=lrr)
##		  return(res)
##	  })


setAs("CNSet", "oligoSetList", function(from, to){
	constructOligoSetListFrom(from)
})



setMethod(OligoSetList, "CNSet", function(object,...){
	constructOligoSetListFrom(object, ...)
})
setMethod(BafLrrSetList, "CNSet", function(object,...){
  constructBafLrrSetListFrom(object, ...)
})





constructOligoSetListFrom <- function(object, ...){
  ##row.index <- seq_len(nrow(object))
  ##col.index <- seq_len(ncol(object))
  is.lds <- ifelse(is(calls(object), "ff_matrix") | is(calls(object), "ffdf"), TRUE, FALSE)
  if(is.lds) stopifnot(isPackageLoaded("ff"))
  b.r <- calculateRBaf(object, ...)
  b <- b.r[["baf"]]
  r <- b.r[["lrr"]]
  j <- match(colnames(r[[1]]), sampleNames(object))
  rns <- lapply(r, rownames)
  fDList <- foreach(featureid=rns) %do%{
    featureData(object)[match(featureid, featureNames(object)), ]
  }
  names(fDList) <- sapply(fDList, function(x) chromosome(x)[1])
  gtPlist <- gtlist <- vector("list", length(r))
  for(i in seq_along(r)){
    gtlist[[i]] <- initializeBigMatrix("call", nr=nrow(r[[i]]), nc=length(j), vmode="integer")
    gtPlist[[i]] <- initializeBigMatrix("callPr", nr=nrow(r[[i]]), nc=length(j), vmode="integer")
    featureid <- rownames(r[[i]])
    ix <- match(featureid, featureNames(object))
    rownames(gtPlist[[i]]) <- rownames(gtlist[[i]]) <- featureid
    colnames(gtPlist[[i]]) <- colnames(gtlist[[i]]) <- colnames(r[[i]])
    for(k in seq_along(j)){
      gtlist[[i]][, k] <- calls(object)[ix, j[k]]
      gtPlist[[i]][, k] <- snpCallProbability(object)[ix, j[k]]
    }
  }
  ad <- AssayDataList(baf=b, copyNumber=r, call=gtlist, callProbability=gtPlist)
  object <- new("oligoSetList",
                assayDataList=ad,
                featureDataList=fDList,
                chromosome=names(fDList),
                phenoData=phenoData(object)[j, ],
                annotation=annotation(object),
                genome=genomeBuild(object))
  return(object)
}



constructBafLrrSetListFrom <- function(object, ...){
	is.lds <- ifelse(is(calls(object), "ff_matrix") | is(calls(object), "ffdf"), TRUE, FALSE)
	if(is.lds) stopifnot(isPackageLoaded("ff"))
	b.r <- calculateRBaf(object, ...)
	b <- b.r[["baf"]]
	r <- b.r[["lrr"]]
	j <- match(colnames(r[[1]]), sampleNames(object))
	rns <- lapply(r, rownames)
	featureid <- NULL
	fDList <- foreach(featureid=rns) %do%{
		featureData(object)[match(featureid, featureNames(object)), ]
	}
	names(fDList) <- sapply(fDList, function(x) chromosome(x)[1])
	ad <- AssayDataList(baf=b, lrr=r)
	object <- new("BafLrrSetList",
		      assayDataList=ad,
		      featureDataList=fDList,
		      chromosome=names(fDList),
		      phenoData=phenoData(object)[j, ],
		      annotation=annotation(object),
		      genome=genomeBuild(object))
	return(object)
}

computeBR <- constructBafLrrSetListFrom
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crlmm
Genotype Calling (CRLMM) and Copy Number Analysis tool for Affymetrix SNP 5.0 and 6.0 and Illumina arrays

R/methods-CNSet.R
In crlmm: Genotype Calling (CRLMM) and Copy Number Analysis tool for Affymetrix SNP 5.0 and 6.0 and Illumina arrays

Defines functions constructBafLrrSetListFrom constructOligoSetListFrom calculateRBafCNSet ACN C3 C2 C1 linearParamElementReplace

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crlmm Genotype Calling (CRLMM) and Copy Number Analysis tool for Affymetrix SNP 5.0 and 6.0 and Illumina arrays

R/methods-CNSet.R In crlmm: Genotype Calling (CRLMM) and Copy Number Analysis tool for Affymetrix SNP 5.0 and 6.0 and Illumina arrays

Defines functions constructBafLrrSetListFrom constructOligoSetListFrom calculateRBafCNSet ACN C3 C2 C1 linearParamElementReplace

Try the crlmm package in your browser

R Package Documentation

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We want your feedback!

crlmm
Genotype Calling (CRLMM) and Copy Number Analysis tool for Affymetrix SNP 5.0 and 6.0 and Illumina arrays

R/methods-CNSet.R
In crlmm: Genotype Calling (CRLMM) and Copy Number Analysis tool for Affymetrix SNP 5.0 and 6.0 and Illumina arrays
