biopipen 0.34.5__py3-none-any.whl → 0.34.7__py3-none-any.whl
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- biopipen/__init__.py +1 -1
- biopipen/ns/tcr.py +6 -3
- biopipen/scripts/scrna/CellTypeAnnotation-celltypist.R +1 -1
- biopipen/scripts/scrna/MarkersFinder.R +3 -1
- biopipen/scripts/scrna/PseudoBulkDEG.R +74 -7
- biopipen/scripts/scrna/ScFGSEA.R +3 -1
- biopipen/scripts/tcr/ScRepCombiningExpression.R +1 -1
- biopipen/scripts/tcr/ScRepLoading.R +12 -0
- {biopipen-0.34.5.dist-info → biopipen-0.34.7.dist-info}/METADATA +1 -1
- {biopipen-0.34.5.dist-info → biopipen-0.34.7.dist-info}/RECORD +12 -12
- {biopipen-0.34.5.dist-info → biopipen-0.34.7.dist-info}/WHEEL +0 -0
- {biopipen-0.34.5.dist-info → biopipen-0.34.7.dist-info}/entry_points.txt +0 -0
biopipen/__init__.py
CHANGED
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@@ -1 +1 @@
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1
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-
__version__ = "0.34.
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1
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+
__version__ = "0.34.7"
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biopipen/ns/tcr.py
CHANGED
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@@ -1682,6 +1682,10 @@ class ScRepLoading(Proc):
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type (choice): The type of the data to load.
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- TCR: T cell receptor data
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- BCR: B cell receptor data
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- auto: Automatically detect the type from the metadata.
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If `auto` is selected, the type will be determined by the presence of
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`TCRData` or `BCRData` columns in the metadata. If both columns are
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present, `TCR` will be selected by default.
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combineTCR (type=json): The extra arguments for `scRepertoire::combineTCR`
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function.
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See also <https://www.borch.dev/uploads/screpertoire/reference/combinetcr>
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@@ -1721,13 +1725,12 @@ class ScRepLoading(Proc):
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output = "outfile:file:{{in.metafile | stem}}.scRep.qs"
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lang = config.lang.rscript
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envs = {
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"type": "
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"type": "auto", # or TCR/BCR
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"combineTCR": {"samples": True},
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"combineBCR": {"samples": True},
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"exclude": ["BCRData", "TCRData", "RNAData"],
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"format": None,
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"tmpdir": config.path.tmpdir,
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-
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}
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script = "file://../scripts/tcr/ScRepLoading.R"
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@@ -1750,7 +1753,7 @@ class ScRepCombiningExpression(Proc):
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Output:
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outfile: The `Seurat` object with the TCR/BCR data combined
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In addition to the meta columns added by
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`scRepertoire::combineExpression()`, a new column `
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`scRepertoire::combineExpression()`, a new column `VDJ_Presence` will be
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added to the metadata. It indicates whether the cell has a TCR/BCR
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sequence or not. The value is `TRUE` if the cell has a TCR/BCR sequence,
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and `FALSE` otherwise.
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@@ -111,7 +111,7 @@ if (file.exists(celltypist_outfile) &&
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command <- paste(command, "-v")
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}
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log$info("Running celltypist:")
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-
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print("- {command}")
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rc <- system(command)
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if (rc != 0) {
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stop("Failed to run celltypist. Check the job.stderr file to see the error message.")
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@@ -165,10 +165,12 @@ post_casing <- function(name, case) {
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if (length(cases) == 0 && name == "Marker Discovery") {
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name <- case$each
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} else {
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name <- paste0(name, " (", case$each, ")")
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}
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for (each in eachs) {
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newname <- paste0(name, "
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newname <- paste0(name, "::", each)
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newcase <- case
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newcase$original_case <- name
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@@ -131,12 +131,14 @@ expand_each <- function(name, case) {
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if (length(cases) == 0 && name == "DEG Analysis") {
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name <- case$each
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} else {
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name <- paste0(name, " (", case$each, ")")
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}
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case$aggregate_by <- unique(c(case$aggregate_by, case$group_by, case$paired_by, case$each))
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for (each in eachs) {
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newname <- paste0(
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newname <- paste0(name, "::", each)
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newcase <- case
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newcase$original_case <- name
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@@ -212,7 +214,52 @@ process_markers <- function(markers, info, case) {
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# markers <- markers %>%
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# mutate(gene = as.character(gene)) %>%
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# arrange(p_val_adj, desc(abs(avg_log2FC)))
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empty <- if (case$enrich_style == "enrichr") {
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data.frame(
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Database = character(0),
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Term = character(0),
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Overlap = character(0),
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P.value = numeric(0),
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Adjusted.P.value = numeric(0),
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Odds.Ratio = numeric(0),
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Combined.Score = numeric(0),
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Genes = character(0),
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Rank = numeric(0)
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)
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} else { # clusterProfiler
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data.frame(
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ID = character(0),
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Description = character(0),
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GeneRatio = character(0),
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BgRatio = character(0),
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Count = integer(0),
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pvalue = numeric(0),
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p.adjust = numeric(0),
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qvalue = numeric(0),
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geneID = character(0),
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Database = character(0)
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)
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}
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if (is.null(markers) || nrow(markers) == 0) {
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if (case$error) {
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stop("Error: No markers found in case '", info$name, "'.")
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} else {
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log$warn("! Warning: No markers found in case '", info$name, "'.")
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reporter$add2(
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list(
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name = "Warning",
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contents = list(list(kind = "error", content = "No markers found.", kind_ = "warning"))),
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hs = c(info$section, info$name),
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hs2 = "DEG Analysis",
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ui = "tabs"
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)
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return(empty)
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}
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}
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markers$gene <- as.character(markers$gene)
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markers$p_val_adj <- as.numeric(markers$p_val_adj)
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markers$log2FC <- as.numeric(markers$log2FC)
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markers <- markers[order(markers$p_val_adj, -abs(markers$log2FC)), ]
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# Save markers
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stop("Error: Not enough significant DEGs with '", case$sigmarkers, "' in case '", info$name, "' found (< 5) for enrichment analysis.")
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} else {
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message <- paste0("Not enough significant DEGs with '", case$sigmarkers, "' found (< 5) for enrichment analysis.")
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log$warn("
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log$warn("! Error: {message}")
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reporter$add2(
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list(
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name = "Warning",
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if (case$error) {
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stop("Error: ", e$message)
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} else {
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log$warn("
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log$warn("! Error: {e$message}")
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reporter$add2(
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list(
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name = "Warning",
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run_case <- function(name) {
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case <- cases[[name]]
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log$info("----------------------------------------")
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log$info("Case: {name} ...")
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case <- extract_vars(
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return(invisible())
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}
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info <- case_info(name, outdir, create = TRUE)
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exprs <- AggregateExpressionPseudobulk(
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srtobj, aggregate_by = aggregate_by, layer = layer, assay = assay,
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subset = subset, log = log
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)
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markers <-
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markers <- tryCatch(
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{
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RunDEGAnalysis(
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exprs, group_by = group_by, ident_1 = ident_1, ident_2 = ident_2,
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paired_by = paired_by, tool = tool, log = log
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)
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}, error = function(e) {
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if (error) {
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stop("Error: ", e$message)
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} else {
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log$warn("! Error: {e$message}")
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reporter$add2(
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list(
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name = "Warning",
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contents = list(list(kind = "error", content = e$message, kind_ = "warning"))),
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hs = c(info$section, info$name),
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hs2 = "DEG Analysis",
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ui = "tabs"
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)
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return(invisible())
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}
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}
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)
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info <- case_info(name, outdir, create = TRUE)
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enrich <- process_markers(markers, info = info, case = list(
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dbs = dbs,
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sigmarkers = sigmarkers,
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biopipen/scripts/scrna/ScFGSEA.R
CHANGED
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if (length(cases) == 0 && name == "GSEA") {
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name <- case$each
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} else {
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name <- paste0(name, " (", case$each, ")")
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}
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for (each in eachs) {
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newname <- paste0(
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newname <- paste0(name, "::", each)
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newcase <- case
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newcase$original_case <- paste0(name, " (all ", case$each,")")
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log$info("Loading metadata ...")
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metadata <- read.table(metafile, header = TRUE, sep = "\t", row.names = NULL, check.names = FALSE)
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if (type == "AUTO") {
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if ("TCRData" %in% colnames(metadata) && "BCRData" %in% colnames(metadata)) {
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log$warn("Both TCRData and BCRData columns found in metadata. Defaulting to TCR.")
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type <- "TCR"
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} else if ("TCRData" %in% colnames(metadata)) {
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type <- "TCR"
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} else if ("BCRData" %in% colnames(metadata)) {
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type <- "BCR"
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} else {
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stop("Error: Neither TCRData nor BCRData column found in metadata.")
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}
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}
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data_column <- ifelse(type == "TCR", "TCRData", "BCRData")
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combine_fn <- ifelse(type == "TCR", combineTCR, combineBCR)
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@@ -1,4 +1,4 @@
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biopipen/__init__.py,sha256=
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biopipen/__init__.py,sha256=vVRUKRt0zUNKxfGQQE5WrQiVWQ-bg4UrgyEGX7LclcA,23
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biopipen/core/__init__.py,sha256=47DEQpj8HBSa-_TImW-5JCeuQeRkm5NMpJWZG3hSuFU,0
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biopipen/core/config.py,sha256=edK5xnDhM8j27srDzsxubi934NMrglLoKrdcC8qsEPk,1069
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biopipen/core/config.toml,sha256=lZV_vbYWk6uqm19ZWJcsZCcSNqAdIfN2fOfamzxZpg4,2148
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@@ -27,7 +27,7 @@ biopipen/ns/scrna_metabolic_landscape.py,sha256=EwLMrsj_pTqvyAgtHLoishjQxCg_j8n5
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biopipen/ns/snp.py,sha256=iXWrw7Lmhf4_ct57HGT7JGTClCXUD4sZ2FzOgsC2pTg,28123
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biopipen/ns/stats.py,sha256=DlPyK5Vsg6ZEkV9SDS3aAw21eXzvOHgqeZDkXPhg7go,20509
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biopipen/ns/tcgamaf.py,sha256=AFbUJIxiMSvsVY3RcHgjRFuMnNh2DG3Mr5slLNEyz6o,1455
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biopipen/ns/tcr.py,sha256=
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biopipen/ns/tcr.py,sha256=XvhbZcVzdJYCjGe61G_EitdRpZyDnyDsaMNPlyH5590,99676
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biopipen/ns/vcf.py,sha256=zjOH2qiSJsHACLmBqV-Tew-mn-peZgvYLAWjTLh7uTI,23823
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biopipen/ns/web.py,sha256=8VY4Xsb8UrzS4IkGUX_84GQP1JG6NcTZrV7f9tA1tUI,5458
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biopipen/reports/bam/CNAClinic.svelte,sha256=D4IxQcgDCPQZMbXog-aZP5iJEQTK2N4i0C60e_iXyfs,213
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@@ -142,7 +142,7 @@ biopipen/scripts/scrna/AnnData2Seurat.R,sha256=wc5PDbK9TkuJtoXXxF4W1ODylWhyfKWd3
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biopipen/scripts/scrna/CCPlotR-patch.R,sha256=KpB8fwacBaWaUNjIidcLUkMShLjS4Gq9UY8LUgIITB0,8369
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biopipen/scripts/scrna/CellCellCommunication.py,sha256=Wg0uFSo0Yt0wq6UT1TBodyK8GtWQXGv7hXRfM665paU,4354
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biopipen/scripts/scrna/CellCellCommunicationPlots.R,sha256=4l2EJVd1y94Nfry8fuRL9OSF6AhS8PGBekimpRUu3s8,1919
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biopipen/scripts/scrna/CellTypeAnnotation-celltypist.R,sha256=
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+
biopipen/scripts/scrna/CellTypeAnnotation-celltypist.R,sha256=CwYR8WWQMf8r7V2CTalG4kxdKnYMtyhpJBe9zP2sQWA,6964
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biopipen/scripts/scrna/CellTypeAnnotation-direct.R,sha256=w3CKRUA9NZfC3TFbU8I35L4XJ6MtVaWX-VnV7ScZlBI,2196
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biopipen/scripts/scrna/CellTypeAnnotation-hitype.R,sha256=vvjhxin4aoA9heecey0dpr6ofirybygY3ApjgtQW89Y,2094
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biopipen/scripts/scrna/CellTypeAnnotation-sccatch.R,sha256=xxB4K1MzBSNQnDxa44s5ExeU67MbncOBf8lGFr7RvwQ,1870
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@@ -155,13 +155,13 @@ biopipen/scripts/scrna/ExprImputation-rmagic.R,sha256=ePgbMZ_3bKbeUrjsMdkdtBM_MS
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biopipen/scripts/scrna/ExprImputation-scimpute.R,sha256=MI_bYfvCDKJsuGntUxfx_-NdrssBoQgL95-DGwJVE5s,1191
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