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R/plot.MassArrayData.R
In MassArray: Analytical Tools for MassArray Data
Defines functions
plot.MassArrayData
Documented in
plot.MassArrayData
plot.MassArrayData <- function(x, y, ...) UseMethod("plot")
plot.MassArrayData <- function (x, ..., collapse=TRUE, bars=TRUE, scale=TRUE, sequence=TRUE, labels=TRUE, colors=TRUE, main=position(x), width=1.5) {
if (!validObject(x)) {
stop("not a valid object of 'MassArrayData'")
}
sequence.tagged <- paste(x$fwd.tag, x$sequence, x$rev.tag, sep="")
N <- nchar(sequence.tagged)
CGs <- CG.positions <- gregexpr("(CG|YG|CR)", sequence.tagged)[[1]]
if (length(CGs) < 1) stop("sequence contains no measurable CpG sites")
## FOR NOW IGNORE GROUPING/SUBSET INFORMATION!!! => ASSUME ALL SAMPLES WITHIN A MassArrayData OBJECT ARE FROM ONE GROUP
CGs.num <- dim(x$CpG.data)[2]
sample.rxns <- unlist(lapply(x$samples, slot, "rxn"))
sample.names <- samples(x)
rxns <- unique(sample.rxns)
num.rxns <- length(rxns)
if (num.rxns < 1) stop("Spectral data contains no reactions")
## GROUP METHYLATION DATA INTO ONE OR MORE SUBSETS OF SAMPLES
if (collapse) {
if (length(x$groups) < 1) x$groups <- rep("", dim(x$CpG.data)[1])
x$groups[which(is.na(x$groups))] <- ""
groups <- length(unique(x$groups))
error.bars <- data.grouped <- matrix(NA, nrow=groups, ncol=CGs.num)
rxn <- rep(NA, groups)
for (i in 1:groups) {
group.i <- which(x$groups == unique(x$groups)[i])
if (length(group.i) > 1) {
error.bars[i, ] <- apply(x$CpG.data[group.i, ], 2, mad, na.rm=TRUE)
data.grouped[i, ] <- apply(x$CpG.data[group.i, ], 2, mean, na.rm=TRUE)
}
else {
error.bars[i, ] <- NA
data.grouped[i, ] <- x$CpG.data[group.i, ]
}
if (length(unique(sample.rxns[group.i])) > 1) {
warning("group ('", unique(x$groups)[i], "') contains multiple rxn variants")
rxn[i] <- "T&C"
}
else {
rxn[i] <- sample.rxns[group.i][1]
}
}
sample.rxns <- rxn
error.bars[which(is.na(error.bars))] <- 0
x$CpG.data <- data.grouped
sample.names <- unique(x$groups)
}
else {
error.bars <- rep(NA, CGs.num)
bars <- FALSE
}
samples.num <- dim(x$CpG.data)[1]
if (scale) {
position.units <- "bp"
CGs <- CGs + 0.5
if (!is.numeric(width)) width <- 1.5
if (is.na(width) | is.nan(width)) width <- 1.5
if (width < 0) width <- abs(width)
width <- min(width, N)
ticks <- pretty(1:N, n=ceiling(N/10))
axis.labels <- pretty(1:N, n=ceiling(N/50))
}
else {
CGs <- 1:length(CGs)
N <- length(CGs)
position.units <- "CG number"
sequence <- FALSE
width <- 0.25
ticks <- 1:N
axis.labels <- 1:N
}
## BEGIN PLOTTING
plot(0, type="n",
xlim=c(1, N),
ylim=c(0, 10), xlab=paste("Nucleotide position (", position.units, ")", sep=""), ylab="",
main=main, axes=FALSE)
axis(1,
labels=axis.labels[match(ticks, axis.labels)],
at=ticks,
cex.lab=0.75, cex.axis=0.75, las=2
)
## DEFINE PLOTTING WINDOW AND SCALING FUNCTION
usr <- par("usr")
scale <- function (x, min1, max1, min2=usr[1], max2=usr[2]) {
return(min2 + (x - min1) * (max2 - min2) / (max1 - min1))
}
if (labels) {
text(CGs,
rep(usr[4], CGs.num),
labels=1:CGs.num,
cex=0.4, col="black", pos=1
)
if (sequence) {
text(1:N,
rep(usr[3], N),
labels=unlist(strsplit(sequence.tagged, "")),
cex=0.2, col="darkgray", pos=3
)
# text((N + 1)/2, usr[3] + 0.035*(usr[4] - usr[3]), labels=position(x), cex=0.25, col="darkgray")
}
}
else {
colors <- FALSE
}
for (i in 1:samples.num) {
if (labels) {
text(usr[1],
scale(samples.num - i + 1.5, 1, samples.num + 1, usr[3] + 0.05*(usr[4] - usr[3]), 0.95*usr[4]),
labels=sample.names[i],
cex=0.4, col="black", pos=4, srt=90
)
}
switch(sample.rxns[i],
"T" = fragments <- x$fragments.T,
"C" = fragments <- x$fragments.C,
fragments <- c(x$fragments.T, x$fragments.C)
)
positions <- unlist(lapply(fragments, slot, "position"))
lengths <- unlist(lapply(fragments, slot, "length"))
cg.fragments <- lapply(CG.positions,
function (x) {
return(which(x >= positions & x < positions + lengths))
}
)
for (j in 1:CGs.num) {
fragment <- fragments[cg.fragments[[j]]]
shading.density <- NA
lty <- "solid"
label.color <- "black"
label.text <- NA
if (colors) {
color.cg <- color.border <- "black"
color.bg <- "peachpuff"
if (all(unlist(lapply(fragment, slot, "CpGs")) > 1)) {
color.bg <- "#FFFFCC"
color.border <- "peachpuff"
# lty <- "dotted"
}
if (all(unlist(lapply(unlist(lapply(fragment, slot, "CG.collision.IDs"), recursive=FALSE), length)) > 0)) {
color.bg <- "#FF9900"
}
}
else {
color.bg <- "#F9F9F9"
color.cg <- color.border <- "black"
}
if (is.na(x$CpG.data[i, j])) {
color.cg <- color.border <- "#CCCCCC"
color.bg <- "white"
shading.density <- NA
# x$CpG.data[i, j] <- 0
}
else if (!any(unlist(lapply(fragment, slot, "assayable")))) {
color.cg <- color.border <- "#BBBBBB"
color.bg <- "#EEEEEE"
}
# else if (colors) {
# color.cg <- color.border <- "black"
# color.bg <- "peachpuff"
# }
# else {
# color.bg <- "#F9F9F9"
# color.cg <- color.border <- "black"
# }
if (all(unlist(lapply(fragment, slot, "required")))) {
# color.border <- "#DD3333"
label.text <- "*"
if (colors) label.color <- "red"
}
if (labels & !is.na(label.text)) {
text(CGs[j],
0.98*usr[4],
labels=label.text,
cex=0.6, col=label.color, pos=1
)
}
rect(CGs[j] - width,
scale(samples.num - i + 1.05, 1, samples.num + 1, usr[3] + 0.05*(usr[4] - usr[3]), 0.95*usr[4]),
CGs[j] + width,
scale(samples.num - i + 1.95, 1, samples.num + 1, usr[3] + 0.05*(usr[4] - usr[3]), 0.95*usr[4]),
border=color.border, col=color.bg, lwd=1, lty=lty, density=shading.density
)
rect(CGs[j] - width,
scale(samples.num - i + 1.05, 1, samples.num + 1, usr[3] + 0.05*(usr[4] - usr[3]), 0.95*usr[4]),
CGs[j] + width,
scale(samples.num - i + scale(x$CpG.data[i, j], 0, 1, 1.05, 1.95), 1, samples.num + 1, usr[3] + 0.05*(usr[4] - usr[3]), 0.95*usr[4]),
border=NA, col=color.cg, lwd=1, lty=lty, density=shading.density
)
## DISPLAY ERROR BARS (IF DESIRED)
if (bars) {
color.cg <- as.numeric(col2rgb(color.cg))+(as.numeric(col2rgb(color.bg))-as.numeric(col2rgb(color.cg)))/2
color.cg <- rgb(color.cg[1], color.cg[2], color.cg[3], maxColorValue=255)
cg <- x$CpG.data[i, j] - c(error.bars[i, j], -error.bars[i, j])
## SKIP ERROR BAR UNLESS THERE IS NON-ZERO DATA TO PLOT
if (is.na(x$CpG.data[i, j]) | is.na(error.bars[i, j]) | (error.bars[i, j] <= 0)) next
## DRAW VERTICAL PORTION OF ERROR BAR
lines(rep(CGs[j], 2),
scale(samples.num - i + scale(c(max(0, cg[1]), min(1, cg[2])), 0, 1, 1.05, 1.95), 1, samples.num + 1, usr[3] + 0.05*(usr[4] - usr[3]), 0.95*usr[4]),
col=color.cg, lwd=1)
## DRAW LOWER DELIMITER OF ERROR BAR
if (cg[1] > 0) {
lines(c(CGs[j] - width/3, CGs[j] + width/3),
scale(samples.num - i + scale(rep(cg[1], 2), 0, 1, 1.05, 1.95), 1, samples.num + 1, usr[3] + 0.05*(usr[4] - usr[3]), 0.95*usr[4]),
col=color.cg, lwd=1)
}
## DRAW UPPER DELIMITER OF ERROR BAR
if (cg[2] < 1) {
lines(c(CGs[j] - width/3, CGs[j] + width/3),
scale(samples.num - i + scale(rep(cg[2], 2), 0, 1, 1.05, 1.95), 1, samples.num + 1, usr[3] + 0.05*(usr[4] - usr[3]), 0.95*usr[4]),
col=color.cg, lwd=1)
}
}
}
}
}
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MassArray documentation built on Nov. 8, 2020, 5:16 p.m.
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Defines functions plot.MassArrayData
Documented in plot.MassArrayData
plot.MassArrayData <- function(x, y, ...) UseMethod("plot")
plot.MassArrayData <- function (x, ..., collapse=TRUE, bars=TRUE, scale=TRUE, sequence=TRUE, labels=TRUE, colors=TRUE, main=position(x), width=1.5) {
if (!validObject(x)) {
stop("not a valid object of 'MassArrayData'")
}
sequence.tagged <- paste(x$fwd.tag, x$sequence, x$rev.tag, sep="")
N <- nchar(sequence.tagged)
CGs <- CG.positions <- gregexpr("(CG|YG|CR)", sequence.tagged)[[1]]
if (length(CGs) < 1) stop("sequence contains no measurable CpG sites")
## FOR NOW IGNORE GROUPING/SUBSET INFORMATION!!! => ASSUME ALL SAMPLES WITHIN A MassArrayData OBJECT ARE FROM ONE GROUP
CGs.num <- dim(x$CpG.data)[2]
sample.rxns <- unlist(lapply(x$samples, slot, "rxn"))
sample.names <- samples(x)
rxns <- unique(sample.rxns)
num.rxns <- length(rxns)
if (num.rxns < 1) stop("Spectral data contains no reactions")
## GROUP METHYLATION DATA INTO ONE OR MORE SUBSETS OF SAMPLES
if (collapse) {
if (length(x$groups) < 1) x$groups <- rep("", dim(x$CpG.data)[1])
x$groups[which(is.na(x$groups))] <- ""
groups <- length(unique(x$groups))
error.bars <- data.grouped <- matrix(NA, nrow=groups, ncol=CGs.num)
rxn <- rep(NA, groups)
for (i in 1:groups) {
group.i <- which(x$groups == unique(x$groups)[i])
if (length(group.i) > 1) {
error.bars[i, ] <- apply(x$CpG.data[group.i, ], 2, mad, na.rm=TRUE)
data.grouped[i, ] <- apply(x$CpG.data[group.i, ], 2, mean, na.rm=TRUE)
}
else {
error.bars[i, ] <- NA
data.grouped[i, ] <- x$CpG.data[group.i, ]
}
if (length(unique(sample.rxns[group.i])) > 1) {
warning("group ('", unique(x$groups)[i], "') contains multiple rxn variants")
rxn[i] <- "T&C"
}
else {
rxn[i] <- sample.rxns[group.i][1]
}
}
sample.rxns <- rxn
error.bars[which(is.na(error.bars))] <- 0
x$CpG.data <- data.grouped
sample.names <- unique(x$groups)
}
else {
error.bars <- rep(NA, CGs.num)
bars <- FALSE
}
samples.num <- dim(x$CpG.data)[1]
if (scale) {
position.units <- "bp"
CGs <- CGs + 0.5
if (!is.numeric(width)) width <- 1.5
if (is.na(width) | is.nan(width)) width <- 1.5
if (width < 0) width <- abs(width)
width <- min(width, N)
ticks <- pretty(1:N, n=ceiling(N/10))
axis.labels <- pretty(1:N, n=ceiling(N/50))
}
else {
CGs <- 1:length(CGs)
N <- length(CGs)
position.units <- "CG number"
sequence <- FALSE
width <- 0.25
ticks <- 1:N
axis.labels <- 1:N
}
## BEGIN PLOTTING
plot(0, type="n",
xlim=c(1, N),
ylim=c(0, 10), xlab=paste("Nucleotide position (", position.units, ")", sep=""), ylab="",
main=main, axes=FALSE)
axis(1,
labels=axis.labels[match(ticks, axis.labels)],
at=ticks,
cex.lab=0.75, cex.axis=0.75, las=2
)
## DEFINE PLOTTING WINDOW AND SCALING FUNCTION
usr <- par("usr")
scale <- function (x, min1, max1, min2=usr[1], max2=usr[2]) {
return(min2 + (x - min1) * (max2 - min2) / (max1 - min1))
}
if (labels) {
text(CGs,
rep(usr[4], CGs.num),
labels=1:CGs.num,
cex=0.4, col="black", pos=1
)
if (sequence) {
text(1:N,
rep(usr[3], N),
labels=unlist(strsplit(sequence.tagged, "")),
cex=0.2, col="darkgray", pos=3
)
# text((N + 1)/2, usr[3] + 0.035*(usr[4] - usr[3]), labels=position(x), cex=0.25, col="darkgray")
}
}
else {
colors <- FALSE
}
for (i in 1:samples.num) {
if (labels) {
text(usr[1],
scale(samples.num - i + 1.5, 1, samples.num + 1, usr[3] + 0.05*(usr[4] - usr[3]), 0.95*usr[4]),
labels=sample.names[i],
cex=0.4, col="black", pos=4, srt=90
)
}
switch(sample.rxns[i],
"T" = fragments <- x$fragments.T,
"C" = fragments <- x$fragments.C,
fragments <- c(x$fragments.T, x$fragments.C)
)
positions <- unlist(lapply(fragments, slot, "position"))
lengths <- unlist(lapply(fragments, slot, "length"))
cg.fragments <- lapply(CG.positions,
function (x) {
return(which(x >= positions & x < positions + lengths))
}
)
for (j in 1:CGs.num) {
fragment <- fragments[cg.fragments[[j]]]
shading.density <- NA
lty <- "solid"
label.color <- "black"
label.text <- NA
if (colors) {
color.cg <- color.border <- "black"
color.bg <- "peachpuff"
if (all(unlist(lapply(fragment, slot, "CpGs")) > 1)) {
color.bg <- "#FFFFCC"
color.border <- "peachpuff"
# lty <- "dotted"
}
if (all(unlist(lapply(unlist(lapply(fragment, slot, "CG.collision.IDs"), recursive=FALSE), length)) > 0)) {
color.bg <- "#FF9900"
}
}
else {
color.bg <- "#F9F9F9"
color.cg <- color.border <- "black"
}
if (is.na(x$CpG.data[i, j])) {
color.cg <- color.border <- "#CCCCCC"
color.bg <- "white"
shading.density <- NA
# x$CpG.data[i, j] <- 0
}
else if (!any(unlist(lapply(fragment, slot, "assayable")))) {
color.cg <- color.border <- "#BBBBBB"
color.bg <- "#EEEEEE"
}
# else if (colors) {
# color.cg <- color.border <- "black"
# color.bg <- "peachpuff"
# }
# else {
# color.bg <- "#F9F9F9"
# color.cg <- color.border <- "black"
# }
if (all(unlist(lapply(fragment, slot, "required")))) {
# color.border <- "#DD3333"
label.text <- "*"
if (colors) label.color <- "red"
}
if (labels & !is.na(label.text)) {
text(CGs[j],
0.98*usr[4],
labels=label.text,
cex=0.6, col=label.color, pos=1
)
}
rect(CGs[j] - width,
scale(samples.num - i + 1.05, 1, samples.num + 1, usr[3] + 0.05*(usr[4] - usr[3]), 0.95*usr[4]),
CGs[j] + width,
scale(samples.num - i + 1.95, 1, samples.num + 1, usr[3] + 0.05*(usr[4] - usr[3]), 0.95*usr[4]),
border=color.border, col=color.bg, lwd=1, lty=lty, density=shading.density
)
rect(CGs[j] - width,
scale(samples.num - i + 1.05, 1, samples.num + 1, usr[3] + 0.05*(usr[4] - usr[3]), 0.95*usr[4]),
CGs[j] + width,
scale(samples.num - i + scale(x$CpG.data[i, j], 0, 1, 1.05, 1.95), 1, samples.num + 1, usr[3] + 0.05*(usr[4] - usr[3]), 0.95*usr[4]),
border=NA, col=color.cg, lwd=1, lty=lty, density=shading.density
)
## DISPLAY ERROR BARS (IF DESIRED)
if (bars) {
color.cg <- as.numeric(col2rgb(color.cg))+(as.numeric(col2rgb(color.bg))-as.numeric(col2rgb(color.cg)))/2
color.cg <- rgb(color.cg[1], color.cg[2], color.cg[3], maxColorValue=255)
cg <- x$CpG.data[i, j] - c(error.bars[i, j], -error.bars[i, j])
## SKIP ERROR BAR UNLESS THERE IS NON-ZERO DATA TO PLOT
if (is.na(x$CpG.data[i, j]) | is.na(error.bars[i, j]) | (error.bars[i, j] <= 0)) next
## DRAW VERTICAL PORTION OF ERROR BAR
lines(rep(CGs[j], 2),
scale(samples.num - i + scale(c(max(0, cg[1]), min(1, cg[2])), 0, 1, 1.05, 1.95), 1, samples.num + 1, usr[3] + 0.05*(usr[4] - usr[3]), 0.95*usr[4]),
col=color.cg, lwd=1)
## DRAW LOWER DELIMITER OF ERROR BAR
if (cg[1] > 0) {
lines(c(CGs[j] - width/3, CGs[j] + width/3),
scale(samples.num - i + scale(rep(cg[1], 2), 0, 1, 1.05, 1.95), 1, samples.num + 1, usr[3] + 0.05*(usr[4] - usr[3]), 0.95*usr[4]),
col=color.cg, lwd=1)
}
## DRAW UPPER DELIMITER OF ERROR BAR
if (cg[2] < 1) {
lines(c(CGs[j] - width/3, CGs[j] + width/3),
scale(samples.num - i + scale(rep(cg[2], 2), 0, 1, 1.05, 1.95), 1, samples.num + 1, usr[3] + 0.05*(usr[4] - usr[3]), 0.95*usr[4]),
col=color.cg, lwd=1)
}
}
}
}
}
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