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R/GNCList-class.R
In GenomicRanges: Representation and manipulation of genomic intervals
Defines functions
findOverlaps_GNCList
GNCList
.extract_groups_from_GenomicRanges
.get_circle_length
Documented in
GNCList
### =========================================================================
### GNCList objects
### -------------------------------------------------------------------------
###
### GNCList is a container for storing a preprocessed GenomicRanges object
### that can be used for fast findOverlaps().
###
setClass("GNCList",
contains="GenomicRanges",
representation(
nclists="list",
granges="GRanges"
)
)
.get_circle_length <- function(x)
{
circle_length <- seqlengths(x)
circle_length[!(isCircular(x) %in% TRUE)] <- NA_integer_
circle_length
}
### - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - -
### Accessors
###
setMethod("granges", "GNCList",
function(x, use.names=TRUE, use.mcols=FALSE)
{
if (!isTRUEorFALSE(use.names))
stop("'use.names' must be TRUE or FALSE")
if (!isTRUEorFALSE(use.mcols))
stop("'use.mcols' must be TRUE or FALSE")
ans <- x@granges
if (!use.names)
names(ans) <- NULL
if (use.mcols)
mcols(ans) <- mcols(x, use.names=FALSE)
ans
}
)
setMethod("length", "GNCList", function(x) length(granges(x)))
setMethod("names", "GNCList", function(x) names(granges(x)))
setMethod("seqnames", "GNCList", function(x) seqnames(granges(x)))
setMethod("start", "GNCList", function(x, ...) start(granges(x)))
setMethod("end", "GNCList", function(x, ...) end(granges(x)))
setMethod("width", "GNCList", function(x) width(granges(x)))
setMethod("ranges", "GNCList",
function(x, use.names=TRUE, use.mcols=FALSE)
ranges(granges(x, use.names=use.names, use.mcols=use.mcols),
use.names=TRUE, use.mcols=use.mcols)
)
setMethod("strand", "GNCList", function(x) strand(granges(x)))
setMethod("seqinfo", "GNCList", function(x) seqinfo(granges(x)))
setAs("GNCList", "GRanges", function(from) granges(from, use.mcols=TRUE))
### - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - -
### Constructor
###
.extract_groups_from_GenomicRanges <- function(x)
splitAsList(seq_along(x) - 1L, seqnames(x))
GNCList <- function(x)
{
if (!is(x, "GenomicRanges"))
stop("'x' must be a GenomicRanges object")
if (!is(x, "GRanges"))
x <- as(x, "GRanges")
ans_mcols <- mcols(x, use.names=FALSE)
mcols(x) <- NULL
x_groups <- .extract_groups_from_GenomicRanges(x)
x_ranges <- IRanges:::.shift_ranges_in_groups_to_first_circle(ranges(x),
x_groups, .get_circle_length(x))
ranges(x) <- x_ranges
x_nclists <- IRanges:::.nclists(x_ranges, x_groups)
new2("GNCList", nclists=x_nclists,
granges=x,
elementMetadata=ans_mcols,
check=FALSE)
}
setAs("GenomicRanges", "GNCList", function(from) GNCList(from))
### - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - -
### Subsetting
###
setMethod("extractROWS", "GNCList",
function(x, i) as(callGeneric(as(x, "GRanges"), i), class(x))
)
### - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - -
### findOverlaps_GNCList()
###
### NOT exported.
findOverlaps_GNCList <- function(query, subject,
maxgap=-1L, minoverlap=0L,
type=c("any", "start", "end", "within", "extend", "equal"),
select=c("all", "first", "last", "arbitrary", "count"),
ignore.strand=FALSE)
{
if (!(is(query, "GenomicRanges") && is(subject, "GenomicRanges")))
stop("'query' and 'subject' must be GenomicRanges objects")
type <- match.arg(type)
select <- match.arg(select)
if (!isTRUEorFALSE(ignore.strand))
stop("'ignore.strand' must be TRUE or FALSE")
si <- merge(seqinfo(query), seqinfo(subject))
q_seqlevels <- seqlevels(query)
s_seqlevels <- seqlevels(subject)
common_seqlevels <- intersect(q_seqlevels, s_seqlevels)
NG <- length(common_seqlevels)
q_group_idx <- match(common_seqlevels, q_seqlevels) # of length NG
s_group_idx <- match(common_seqlevels, s_seqlevels) # of length NG
## Extract 'q_groups' and 's_groups' (both of length NG).
q_groups <- .extract_groups_from_GenomicRanges(query)[q_group_idx]
s_groups <- .extract_groups_from_GenomicRanges(subject)[s_group_idx]
## Extract 'nclists' and 'nclist_is_q' (both of length NG).
if (is(subject, "GNCList")) {
nclists <- subject@nclists[s_group_idx]
nclist_is_q <- rep.int(FALSE, NG)
} else if (is(query, "GNCList")) {
nclists <- query@nclists[q_group_idx]
nclist_is_q <- rep.int(TRUE, NG)
} else {
## We'll do "on-the-fly preprocessing".
nclists <- vector(mode="list", length=NG)
nclist_is_q <- rep.int(NA, NG)
}
## Extract 'circle_length' (of length NG).
circle_length <- .get_circle_length(si)[q_group_idx]
## Extract 'q_space' and 's_space'.
if (ignore.strand) {
q_space <- s_space <- NULL
} else {
q_space <- as.integer(strand(query)) - 3L
s_space <- as.integer(strand(subject)) - 3L
}
## GO!
IRanges:::find_overlaps_in_groups_NCList(
ranges(query), q_space, q_groups,
ranges(subject), s_space, s_groups,
nclists, nclist_is_q,
maxgap, minoverlap, type, select, circle_length)
}
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GenomicRanges documentation built on Nov. 8, 2020, 5:46 p.m.
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Defines functions findOverlaps_GNCList GNCList .extract_groups_from_GenomicRanges .get_circle_length
Documented in GNCList
### =========================================================================
### GNCList objects
### -------------------------------------------------------------------------
###
### GNCList is a container for storing a preprocessed GenomicRanges object
### that can be used for fast findOverlaps().
###
setClass("GNCList",
contains="GenomicRanges",
representation(
nclists="list",
granges="GRanges"
)
)
.get_circle_length <- function(x)
{
circle_length <- seqlengths(x)
circle_length[!(isCircular(x) %in% TRUE)] <- NA_integer_
circle_length
}
### - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - -
### Accessors
###
setMethod("granges", "GNCList",
function(x, use.names=TRUE, use.mcols=FALSE)
{
if (!isTRUEorFALSE(use.names))
stop("'use.names' must be TRUE or FALSE")
if (!isTRUEorFALSE(use.mcols))
stop("'use.mcols' must be TRUE or FALSE")
ans <- x@granges
if (!use.names)
names(ans) <- NULL
if (use.mcols)
mcols(ans) <- mcols(x, use.names=FALSE)
ans
}
)
setMethod("length", "GNCList", function(x) length(granges(x)))
setMethod("names", "GNCList", function(x) names(granges(x)))
setMethod("seqnames", "GNCList", function(x) seqnames(granges(x)))
setMethod("start", "GNCList", function(x, ...) start(granges(x)))
setMethod("end", "GNCList", function(x, ...) end(granges(x)))
setMethod("width", "GNCList", function(x) width(granges(x)))
setMethod("ranges", "GNCList",
function(x, use.names=TRUE, use.mcols=FALSE)
ranges(granges(x, use.names=use.names, use.mcols=use.mcols),
use.names=TRUE, use.mcols=use.mcols)
)
setMethod("strand", "GNCList", function(x) strand(granges(x)))
setMethod("seqinfo", "GNCList", function(x) seqinfo(granges(x)))
setAs("GNCList", "GRanges", function(from) granges(from, use.mcols=TRUE))
### - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - -
### Constructor
###
.extract_groups_from_GenomicRanges <- function(x)
splitAsList(seq_along(x) - 1L, seqnames(x))
GNCList <- function(x)
{
if (!is(x, "GenomicRanges"))
stop("'x' must be a GenomicRanges object")
if (!is(x, "GRanges"))
x <- as(x, "GRanges")
ans_mcols <- mcols(x, use.names=FALSE)
mcols(x) <- NULL
x_groups <- .extract_groups_from_GenomicRanges(x)
x_ranges <- IRanges:::.shift_ranges_in_groups_to_first_circle(ranges(x),
x_groups, .get_circle_length(x))
ranges(x) <- x_ranges
x_nclists <- IRanges:::.nclists(x_ranges, x_groups)
new2("GNCList", nclists=x_nclists,
granges=x,
elementMetadata=ans_mcols,
check=FALSE)
}
setAs("GenomicRanges", "GNCList", function(from) GNCList(from))
### - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - -
### Subsetting
###
setMethod("extractROWS", "GNCList",
function(x, i) as(callGeneric(as(x, "GRanges"), i), class(x))
)
### - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - - -
### findOverlaps_GNCList()
###
### NOT exported.
findOverlaps_GNCList <- function(query, subject,
maxgap=-1L, minoverlap=0L,
type=c("any", "start", "end", "within", "extend", "equal"),
select=c("all", "first", "last", "arbitrary", "count"),
ignore.strand=FALSE)
{
if (!(is(query, "GenomicRanges") && is(subject, "GenomicRanges")))
stop("'query' and 'subject' must be GenomicRanges objects")
type <- match.arg(type)
select <- match.arg(select)
if (!isTRUEorFALSE(ignore.strand))
stop("'ignore.strand' must be TRUE or FALSE")
si <- merge(seqinfo(query), seqinfo(subject))
q_seqlevels <- seqlevels(query)
s_seqlevels <- seqlevels(subject)
common_seqlevels <- intersect(q_seqlevels, s_seqlevels)
NG <- length(common_seqlevels)
q_group_idx <- match(common_seqlevels, q_seqlevels) # of length NG
s_group_idx <- match(common_seqlevels, s_seqlevels) # of length NG
## Extract 'q_groups' and 's_groups' (both of length NG).
q_groups <- .extract_groups_from_GenomicRanges(query)[q_group_idx]
s_groups <- .extract_groups_from_GenomicRanges(subject)[s_group_idx]
## Extract 'nclists' and 'nclist_is_q' (both of length NG).
if (is(subject, "GNCList")) {
nclists <- subject@nclists[s_group_idx]
nclist_is_q <- rep.int(FALSE, NG)
} else if (is(query, "GNCList")) {
nclists <- query@nclists[q_group_idx]
nclist_is_q <- rep.int(TRUE, NG)
} else {
## We'll do "on-the-fly preprocessing".
nclists <- vector(mode="list", length=NG)
nclist_is_q <- rep.int(NA, NG)
}
## Extract 'circle_length' (of length NG).
circle_length <- .get_circle_length(si)[q_group_idx]
## Extract 'q_space' and 's_space'.
if (ignore.strand) {
q_space <- s_space <- NULL
} else {
q_space <- as.integer(strand(query)) - 3L
s_space <- as.integer(strand(subject)) - 3L
}
## GO!
IRanges:::find_overlaps_in_groups_NCList(
ranges(query), q_space, q_groups,
ranges(subject), s_space, s_groups,
nclists, nclist_is_q,
maxgap, minoverlap, type, select, circle_length)
}
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We want your feedback!
Note that we can't provide technical support on individual packages. You should contact the package authors for that.
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