Nothing
R/Show_database_information.R
In Uniquorn: Identification of cancer cell lines based on their weighted mutational/ variational fingerprint
Defines functions
read_library_names
show_which_ccls_contain_variant
show_contained_variants_for_ccl
show_contained_variants_in_library
show_contained_ccls
Documented in
read_library_names
show_contained_ccls
show_contained_variants_for_ccl
show_contained_variants_in_library
show_which_ccls_contain_variant
#' show_contained_ccls
#'
#' This function displays the names, amount of mutations and the overall
#' weight of the mutations of all contained cancer cell line fingerprints
#' for a chosen reference genome and optional library.
#'
#' @param ref_gen a character vector specifying the reference genome version.
#' All training sets are associated with a reference genome version.
#' Default is \code{"GRCH37"}.
#' @param verbose Should DB informations be printed?
#' @return R table which contains identifiers of all cancer cell line samples
#' which match the specified parameters (reference genome and library).
#' @usage
#' show_contained_ccls(ref_gen, verbose)
#' @examples
#' ## Show all contained cancer cell lines for reference GRCH37:
#' show_contained_ccls(ref_gen = "GRCH37", verbose = TRUE)
#' @import GenomicRanges stringr
#' @export
show_contained_ccls = function(
ref_gen = "GRCH37",
verbose = TRUE
){
package_path = system.file("", package = "Uniquorn")
library_path = paste( c( package_path,"/Libraries/",ref_gen),
sep ="", collapse= "")
if ( ! dir.exists( library_path ))
stop("No libraries found!")
libraries = list.dirs(library_path, full.names = FALSE)
libraries = libraries[ libraries != ""]
ccls_all <<- data.frame(
"CCL" = as.character(),
"Library" = as.character(),
"W0" = as.character(),
"W25" = as.character(),
"W05" = as.character(),
"W1" = as.character()
)
for (library_name in libraries){
stats_path = paste( c( library_path,"/",library_name,
"/CCL_List_Uniquorn_DB.RData"), sep ="", collapse= "")
g_library = readRDS(stats_path)
cl_id_no_library = str_replace_all( g_library$CCL, pattern =
paste("_", library_name, sep = ""), "" )
g_library$CCL = cl_id_no_library
if (verbose) {
message(library_name," amount CCLs: ",
as.character(nrow(g_library)))
}
g_library$Library = rep(library_name, nrow(g_library))
g_library = g_library[c("CCL","Library","W0","W25","W05","W1")]
ccls_all <<- rbind(ccls_all, g_library )
}
return(ccls_all)
}
#' All variants contained in reference library
#'
#' This function shows all variants contained in a reference library
#' for a given inclusion weight. Default inclusion weight is 0
#' (all variants).
#'
#' @param ref_gen a character vector specifying the reference genome
#' version. All training sets are associated with a reference genome version.
#' Default is \code{"GRCH37"}.
#' @param library_name Name of the reference library.
#' @param mutational_weight_inclusion_threshold Include only mutations
#' with a weight of at least x. Range: 0.0 to 1.0. 1 = unique to CL.
#' ~0 = found in many CL samples.
#' @usage
#' show_contained_variants_in_library(
#' ref_gen,
#' library_name,
#' mutational_weight_inclusion_threshold
#' )
#' @import stringr
#' @examples
#' ## Show all variants contained in reference library CELLMINER
#' show_contained_variants_in_library(
#' ref_gen = "GRCH37",
#' library_name = "CELLMINER",
#' mutational_weight_inclusion_threshold = 0
#' )
#' @return Returns a GenomicRanges object that contains the variants
#' @export
show_contained_variants_in_library = function(
ref_gen = "GRCH37",
library_name,
mutational_weight_inclusion_threshold = 0
){
message("Entered reference genome: ", ref_gen,
". Entered library name: ", library_name)
package_path = system.file("", package = "Uniquorn")
library_path = paste(
c(package_path, "/Libraries/", ref_gen), sep = "", collapse= ""
)
if ( ! dir.exists( library_path ))
stop("No libraries found!")
libraries = list.dirs(library_path,full.names = FALSE)
libraries = libraries[ libraries != ""]
if (! (library_name %in% libraries ))
stop("Could not find library!")
g_mat = read_mutation_grange_objects(
library_name = library_name,
ref_gen = ref_gen,
mutational_weight_inclusion_threshold =
mutational_weight_inclusion_threshold,
test_mode = FALSE
)
return(g_mat)
}
#' Variants In Cancer Cell Line
#'
#' This function shows all mutations present in the database
#' for a selected cancer cell line and reference genome.
#'
#' @param name_ccl a character vector giving the identifier
#' of the cancer cell line for which mutations will be shown.
#' @param ref_gen a character vector specifying the reference
#' genome version. All training sets are associated with a
#' reference genome version. Default is \code{"GRCH37"}.
#' @param library_name Name of the reference library
#' @param mutational_weight_inclusion_threshold Include only mutations
#' with a weight of at least x. Range: 0.0 to 1.0. 1= unique to CL.
#' ~0 = found in many CCL samples.
#' @import stringr
#' @usage
#' show_contained_variants_for_ccl(
#' name_ccl,
#' ref_gen,
#' library_name,
#' mutational_weight_inclusion_threshold
#' )
#' @examples
#' ## Show all mutations for Cancer Cell Line 'SK_OV_3'
#' show_contained_variants_for_ccl(
#' name_ccl = "SK_OV_3",
#' ref_gen = "GRCH37",
#' library_name = "CELLMINER",
#' mutational_weight_inclusion_threshold = 0
#' )
#' @return GenomicRanges object that contains the ccl's variants
#' @export
show_contained_variants_for_ccl = function(
name_ccl,
ref_gen = "GRCH37",
library_name,
mutational_weight_inclusion_threshold = 0
){
message("Entered reference genome: ", ref_gen,
". Entered library name: ", library_name,
". Entered name of ccl: ", name_ccl)
package_path = system.file("", package = "Uniquorn")
library_path = paste(c(package_path, "/Libraries/", ref_gen),
sep ="", collapse= "")
if ( ! dir.exists( library_path ))
stop("No libraries found!")
libraries = list.dirs(library_path,full.names = FALSE)
libraries = libraries[ libraries != ""]
if (! (library_name %in% libraries ))
stop("Could not find library!")
g_mat = read_mutation_grange_objects(
library_name = library_name,
ref_gen = ref_gen,
mutational_weight_inclusion_threshold =
mutational_weight_inclusion_threshold,
test_mode = FALSE
)
g_query_index = stringr::str_detect(g_mat$Member_CCLs, pattern = name_ccl)
g_query = g_mat[g_query_index,]
return(g_query)
}
#' Cancer cell lines with specific variant
#'
#' This function displays all cancer cell lines in the database which
#' contain a specified variant. Utilizes closed interval coordinates.
#'
#' @param start Start coordinate
#' @param end Stop coordinate
#' @param chromosome Chromosome, 'chr' prefixes are ignored
#' @param ref_gen a character vector specifying the reference genome
#' version. All training sets are associated with a reference genome
#' version. Default is \code{"GRCH37"}.
#' @param library_name Name of the reference library
#' @param mutational_weight_inclusion_threshold Include only mutations
#' with a weight of at least x. Range: 0.0 to 1.0. 1= unique to CL.
#' ~0 = found in many CCL samples.
#' @import stringr
#' @importFrom IRanges IRanges
#' @importFrom IRanges subsetByOverlaps
#' @usage
#' show_which_ccls_contain_variant(
#' start,
#' end,
#' chromosome,
#' ref_gen,
#' library_name,
#' mutational_weight_inclusion_threshold
#' )
#' @examples
#' show_which_ccls_contain_variant(
#' start = 92030762,
#' end = 92030762,
#' chromosome = 8,
#' ref_gen = "GRCH37",
#' library_name = "CELLMINER",
#' mutational_weight_inclusion_threshold = 0
#' )
#' @return Returns a GenomicRanges object that contains the variant if present.
#' Member ccls can be found in the $Member_ccl vector
#' @export
show_which_ccls_contain_variant = function(
start,
end,
chromosome,
ref_gen = "GRCH37",
library_name,
mutational_weight_inclusion_threshold = 0
){
message("Entered reference genome: ", ref_gen,
". Entered library name: ", library_name)
package_path = system.file("", package = "Uniquorn")
library_path = paste(
c(package_path, "/Libraries/", ref_gen), sep ="", collapse= ""
)
if ( ! dir.exists( library_path ))
stop("No libraries found!")
libraries = list.dirs(library_path,full.names = FALSE)
libraries = libraries[ libraries != ""]
if (! (library_name %in% libraries ))
stop("Could not find library!")
g_mat = read_mutation_grange_objects(
library_name = library_name,
ref_gen = ref_gen,
mutational_weight_inclusion_threshold =
mutational_weight_inclusion_threshold,
test_mode = FALSE
)
chromosome = stringr::str_to_upper(chromosome)
chroms = stringr::str_replace( chromosome, pattern = "^CHR" , "")
g_query = GenomicRanges::GRanges(
seqnames = c( chroms ),
IRanges::IRanges(
start = as.integer( c(start) ),
end = as.integer( c(end) )
)
)
g_query = IRanges::subsetByOverlaps(g_mat, g_query)
return(g_query)
}
#' Library Name Reader
#'
#' This function procides information on the reference library names
#'
#' @param ref_gen a character vector specifying the reference genome
#' version. All training sets are associated with a reference genome
#' version. Default is \code{"GRCH37"}.
#' @import stringr
#' @usage
#' read_library_names(ref_gen)
#' @examples
#' read_library_names(ref_gen = "GRCH37")
#' @return Returns a character vector of the contained libraries
#' @export
read_library_names = function(
ref_gen
){
package_path = system.file("", package = "Uniquorn")
library_path = paste(c(package_path, "/Libraries/", ref_gen, "/"),
sep ="", collapse= "")
library_names = list.dirs(library_path, full.names = FALSE)
library_names = library_names[library_names!= ""]
return(library_names)
}
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Defines functions read_library_names show_which_ccls_contain_variant show_contained_variants_for_ccl show_contained_variants_in_library show_contained_ccls
Documented in read_library_names show_contained_ccls show_contained_variants_for_ccl show_contained_variants_in_library show_which_ccls_contain_variant
#' show_contained_ccls
#'
#' This function displays the names, amount of mutations and the overall
#' weight of the mutations of all contained cancer cell line fingerprints
#' for a chosen reference genome and optional library.
#'
#' @param ref_gen a character vector specifying the reference genome version.
#' All training sets are associated with a reference genome version.
#' Default is \code{"GRCH37"}.
#' @param verbose Should DB informations be printed?
#' @return R table which contains identifiers of all cancer cell line samples
#' which match the specified parameters (reference genome and library).
#' @usage
#' show_contained_ccls(ref_gen, verbose)
#' @examples
#' ## Show all contained cancer cell lines for reference GRCH37:
#' show_contained_ccls(ref_gen = "GRCH37", verbose = TRUE)
#' @import GenomicRanges stringr
#' @export
show_contained_ccls = function(
ref_gen = "GRCH37",
verbose = TRUE
){
package_path = system.file("", package = "Uniquorn")
library_path = paste( c( package_path,"/Libraries/",ref_gen),
sep ="", collapse= "")
if ( ! dir.exists( library_path ))
stop("No libraries found!")
libraries = list.dirs(library_path, full.names = FALSE)
libraries = libraries[ libraries != ""]
ccls_all <<- data.frame(
"CCL" = as.character(),
"Library" = as.character(),
"W0" = as.character(),
"W25" = as.character(),
"W05" = as.character(),
"W1" = as.character()
)
for (library_name in libraries){
stats_path = paste( c( library_path,"/",library_name,
"/CCL_List_Uniquorn_DB.RData"), sep ="", collapse= "")
g_library = readRDS(stats_path)
cl_id_no_library = str_replace_all( g_library$CCL, pattern =
paste("_", library_name, sep = ""), "" )
g_library$CCL = cl_id_no_library
if (verbose) {
message(library_name," amount CCLs: ",
as.character(nrow(g_library)))
}
g_library$Library = rep(library_name, nrow(g_library))
g_library = g_library[c("CCL","Library","W0","W25","W05","W1")]
ccls_all <<- rbind(ccls_all, g_library )
}
return(ccls_all)
}
#' All variants contained in reference library
#'
#' This function shows all variants contained in a reference library
#' for a given inclusion weight. Default inclusion weight is 0
#' (all variants).
#'
#' @param ref_gen a character vector specifying the reference genome
#' version. All training sets are associated with a reference genome version.
#' Default is \code{"GRCH37"}.
#' @param library_name Name of the reference library.
#' @param mutational_weight_inclusion_threshold Include only mutations
#' with a weight of at least x. Range: 0.0 to 1.0. 1 = unique to CL.
#' ~0 = found in many CL samples.
#' @usage
#' show_contained_variants_in_library(
#' ref_gen,
#' library_name,
#' mutational_weight_inclusion_threshold
#' )
#' @import stringr
#' @examples
#' ## Show all variants contained in reference library CELLMINER
#' show_contained_variants_in_library(
#' ref_gen = "GRCH37",
#' library_name = "CELLMINER",
#' mutational_weight_inclusion_threshold = 0
#' )
#' @return Returns a GenomicRanges object that contains the variants
#' @export
show_contained_variants_in_library = function(
ref_gen = "GRCH37",
library_name,
mutational_weight_inclusion_threshold = 0
){
message("Entered reference genome: ", ref_gen,
". Entered library name: ", library_name)
package_path = system.file("", package = "Uniquorn")
library_path = paste(
c(package_path, "/Libraries/", ref_gen), sep = "", collapse= ""
)
if ( ! dir.exists( library_path ))
stop("No libraries found!")
libraries = list.dirs(library_path,full.names = FALSE)
libraries = libraries[ libraries != ""]
if (! (library_name %in% libraries ))
stop("Could not find library!")
g_mat = read_mutation_grange_objects(
library_name = library_name,
ref_gen = ref_gen,
mutational_weight_inclusion_threshold =
mutational_weight_inclusion_threshold,
test_mode = FALSE
)
return(g_mat)
}
#' Variants In Cancer Cell Line
#'
#' This function shows all mutations present in the database
#' for a selected cancer cell line and reference genome.
#'
#' @param name_ccl a character vector giving the identifier
#' of the cancer cell line for which mutations will be shown.
#' @param ref_gen a character vector specifying the reference
#' genome version. All training sets are associated with a
#' reference genome version. Default is \code{"GRCH37"}.
#' @param library_name Name of the reference library
#' @param mutational_weight_inclusion_threshold Include only mutations
#' with a weight of at least x. Range: 0.0 to 1.0. 1= unique to CL.
#' ~0 = found in many CCL samples.
#' @import stringr
#' @usage
#' show_contained_variants_for_ccl(
#' name_ccl,
#' ref_gen,
#' library_name,
#' mutational_weight_inclusion_threshold
#' )
#' @examples
#' ## Show all mutations for Cancer Cell Line 'SK_OV_3'
#' show_contained_variants_for_ccl(
#' name_ccl = "SK_OV_3",
#' ref_gen = "GRCH37",
#' library_name = "CELLMINER",
#' mutational_weight_inclusion_threshold = 0
#' )
#' @return GenomicRanges object that contains the ccl's variants
#' @export
show_contained_variants_for_ccl = function(
name_ccl,
ref_gen = "GRCH37",
library_name,
mutational_weight_inclusion_threshold = 0
){
message("Entered reference genome: ", ref_gen,
". Entered library name: ", library_name,
". Entered name of ccl: ", name_ccl)
package_path = system.file("", package = "Uniquorn")
library_path = paste(c(package_path, "/Libraries/", ref_gen),
sep ="", collapse= "")
if ( ! dir.exists( library_path ))
stop("No libraries found!")
libraries = list.dirs(library_path,full.names = FALSE)
libraries = libraries[ libraries != ""]
if (! (library_name %in% libraries ))
stop("Could not find library!")
g_mat = read_mutation_grange_objects(
library_name = library_name,
ref_gen = ref_gen,
mutational_weight_inclusion_threshold =
mutational_weight_inclusion_threshold,
test_mode = FALSE
)
g_query_index = stringr::str_detect(g_mat$Member_CCLs, pattern = name_ccl)
g_query = g_mat[g_query_index,]
return(g_query)
}
#' Cancer cell lines with specific variant
#'
#' This function displays all cancer cell lines in the database which
#' contain a specified variant. Utilizes closed interval coordinates.
#'
#' @param start Start coordinate
#' @param end Stop coordinate
#' @param chromosome Chromosome, 'chr' prefixes are ignored
#' @param ref_gen a character vector specifying the reference genome
#' version. All training sets are associated with a reference genome
#' version. Default is \code{"GRCH37"}.
#' @param library_name Name of the reference library
#' @param mutational_weight_inclusion_threshold Include only mutations
#' with a weight of at least x. Range: 0.0 to 1.0. 1= unique to CL.
#' ~0 = found in many CCL samples.
#' @import stringr
#' @importFrom IRanges IRanges
#' @importFrom IRanges subsetByOverlaps
#' @usage
#' show_which_ccls_contain_variant(
#' start,
#' end,
#' chromosome,
#' ref_gen,
#' library_name,
#' mutational_weight_inclusion_threshold
#' )
#' @examples
#' show_which_ccls_contain_variant(
#' start = 92030762,
#' end = 92030762,
#' chromosome = 8,
#' ref_gen = "GRCH37",
#' library_name = "CELLMINER",
#' mutational_weight_inclusion_threshold = 0
#' )
#' @return Returns a GenomicRanges object that contains the variant if present.
#' Member ccls can be found in the $Member_ccl vector
#' @export
show_which_ccls_contain_variant = function(
start,
end,
chromosome,
ref_gen = "GRCH37",
library_name,
mutational_weight_inclusion_threshold = 0
){
message("Entered reference genome: ", ref_gen,
". Entered library name: ", library_name)
package_path = system.file("", package = "Uniquorn")
library_path = paste(
c(package_path, "/Libraries/", ref_gen), sep ="", collapse= ""
)
if ( ! dir.exists( library_path ))
stop("No libraries found!")
libraries = list.dirs(library_path,full.names = FALSE)
libraries = libraries[ libraries != ""]
if (! (library_name %in% libraries ))
stop("Could not find library!")
g_mat = read_mutation_grange_objects(
library_name = library_name,
ref_gen = ref_gen,
mutational_weight_inclusion_threshold =
mutational_weight_inclusion_threshold,
test_mode = FALSE
)
chromosome = stringr::str_to_upper(chromosome)
chroms = stringr::str_replace( chromosome, pattern = "^CHR" , "")
g_query = GenomicRanges::GRanges(
seqnames = c( chroms ),
IRanges::IRanges(
start = as.integer( c(start) ),
end = as.integer( c(end) )
)
)
g_query = IRanges::subsetByOverlaps(g_mat, g_query)
return(g_query)
}
#' Library Name Reader
#'
#' This function procides information on the reference library names
#'
#' @param ref_gen a character vector specifying the reference genome
#' version. All training sets are associated with a reference genome
#' version. Default is \code{"GRCH37"}.
#' @import stringr
#' @usage
#' read_library_names(ref_gen)
#' @examples
#' read_library_names(ref_gen = "GRCH37")
#' @return Returns a character vector of the contained libraries
#' @export
read_library_names = function(
ref_gen
){
package_path = system.file("", package = "Uniquorn")
library_path = paste(c(package_path, "/Libraries/", ref_gen, "/"),
sep ="", collapse= "")
library_names = list.dirs(library_path, full.names = FALSE)
library_names = library_names[library_names!= ""]
return(library_names)
}
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