Mercurial > repos > bgruening > music_construct_eset
changeset 2:7902cd31b9b5 draft
"planemo upload for repository https://github.com/galaxyproject/tools-iuc/tree/master/tools/music/ commit 20f8561478535013e111d982b99639f48f1bea79"
author | bgruening |
---|---|
date | Sat, 29 Jan 2022 12:52:10 +0000 |
parents | be91cb6f48e7 |
children | 7ffaa0968da3 |
files | construct_eset.xml macros.xml scripts/dendrogram.R scripts/estimateprops.R scripts/inspect.R test-data/default_output_no_disease.pdf test-data/mouse_scrna_exprs.tabular test-data/mouse_scrna_pheno.tabular |
diffstat | 8 files changed, 341 insertions(+), 111 deletions(-) [+] |
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--- a/construct_eset.xml Fri Nov 26 15:55:11 2021 +0000 +++ b/construct_eset.xml Sat Jan 29 12:52:10 2022 +0000 @@ -33,13 +33,13 @@ ## - This file is the only non-optional parameter exprs_file = '$exprs_file' exprs = as.matrix(read.table(exprs_file, header = T, sep = "\t", - row.names = 1, as.is = T)) + row.names = 1, as.is = T, check.names=FALSE)) ## Phenotype Data ## S rows of samples, and V columns of covariates (e.g. sex, age, etc.) pdata = NULL #if '$pdata_file': pdata_file = '$pdata_file' -pdata = read.table(pdata_file, row.names = 1, header = T, sep = "\t", as.is=T) +pdata = read.table(pdata_file, row.names = 1, header = T, sep = "\t", as.is=T, check.names=FALSE) #end if ## Annotation and Feature Data, or just a string for type of chip used annotation = null_str_vec('$annotation') @@ -158,10 +158,20 @@ </inputs> <outputs> <data name="out_txt" format="txt" label="${tool.name} on ${on_string}: General Info" /> - <data name="out_rds" format="rdata.eset" label="${tool.name} on ${on_string}: RData ESet Object" /> + <data name="out_rds" format="@RDATATYPE@" label="${tool.name} on ${on_string}: RData ESet Object" /> </outputs> <tests> <test expect_num_outputs="2" > + <!-- Simple object --> + <param name="exprs_file" value="mouse_scrna_exprs.tabular" /> + <param name="pdata_file" value="mouse_scrna_pheno.tabular" /> + <output name="out_txt"> + <assert_contents> + <has_text text="assayData: 100 features, 100 samples " /> + </assert_contents> + </output> + </test> + <test expect_num_outputs="2" > <!-- Values from the manual --> <param name="exprs_file" value="array.tsv" /> <param name="pdata_file" value="pheno.tsv" />
--- a/macros.xml Fri Nov 26 15:55:11 2021 +0000 +++ b/macros.xml Sat Jan 29 12:52:10 2022 +0000 @@ -1,9 +1,14 @@ <macros> - <token name="@VERSION_SUFFIX@">1</token> + <token name="@VERSION_SUFFIX@">2</token> <!-- The ESet inspector/constructor and MuSiC tool can have independent Galaxy versions but should reference the same package version always. --> <token name="@TOOL_VERSION@">0.1.1</token> + <token name="@RDATATYPE@">rdata</token> + <!-- Below is disabled until Galaxy supports it. Still not present + in 21.09 + <token name="@RDATATYPE@">rdata.eset</token> + --> <xml name="requirements"> <requirements> <requirement type="package" version="@TOOL_VERSION@" >music-deconvolution</requirement>
--- a/scripts/dendrogram.R Fri Nov 26 15:55:11 2021 +0000 +++ b/scripts/dendrogram.R Sat Jan 29 12:52:10 2022 +0000 @@ -10,7 +10,7 @@ if (lfile == "None") { return(NULL) } - return(read.table(file = lfile, header = FALSE, + return(read.table(file = lfile, header = FALSE, check.names = FALSE, stringsAsFactors = FALSE)$V1) }
--- a/scripts/estimateprops.R Fri Nov 26 15:55:11 2021 +0000 +++ b/scripts/estimateprops.R Sat Jan 29 12:52:10 2022 +0000 @@ -17,13 +17,21 @@ estimated_music_props <- est_prop$Est.prop.weighted estimated_nnls_props <- est_prop$Est.prop.allgene +scale_yaxes <- function(gplot, value) { + if (is.na(value)) { + gplot + } else { + gplot + scale_y_continuous(lim = c(0, value)) + } +} + ## Show different in estimation methods ## Jitter plot of estimated cell type proportions -jitter_fig <- Jitter_Est( +jitter_fig <- scale_yaxes(Jitter_Est( list(data.matrix(estimated_music_props), data.matrix(estimated_nnls_props)), method.name = methods, title = "Jitter plot of Est Proportions", - size = 2, alpha = 0.7) + theme_minimal() + size = 2, alpha = 0.7) + theme_minimal(), maxyscale) ## Make a Plot @@ -42,11 +50,6 @@ message(celltypes) } -if (phenotype_target_threshold == -99) { - phenotype_target_threshold <- -Inf - message("phenotype target threshold set to -Inf") -} - if (is.null(phenotype_factors)) { phenotype_factors <- colnames(pData(bulk_eset)) } @@ -54,67 +57,94 @@ phenotype_factors <- phenotype_factors[ !(phenotype_factors %in% phenotype_factors_always_exclude)] message("Phenotype Factors to use:") -message(phenotype_factors) - +message(paste0(phenotype_factors, collapse = ", ")) m_prop$CellType <- factor(m_prop$CellType, levels = celltypes) # nolint m_prop$Method <- factor(rep(methods, each = nrow(estimated_music_props_flat)), # nolint levels = methods) -m_prop$Disease_factor <- rep(bulk_eset[[phenotype_target]], 2 * length(celltypes)) # nolint -m_prop <- m_prop[!is.na(m_prop$Disease_factor), ] -## Generate a TRUE/FALSE table of Normal == 1 and Disease == 2 -sample_groups <- c("Normal", sample_disease_group) -m_prop$Disease <- factor(sample_groups[(m_prop$Disease_factor > phenotype_target_threshold) + 1], # nolint - levels = sample_groups) + +if (use_disease_factor) { + + if (phenotype_target_threshold == -99) { + phenotype_target_threshold <- -Inf + message("phenotype target threshold set to -Inf") + } + + m_prop$Disease_factor <- rep(bulk_eset[[phenotype_target]], 2 * length(celltypes)) # nolint + m_prop <- m_prop[!is.na(m_prop$Disease_factor), ] + ## Generate a TRUE/FALSE table of Normal == 1 and Disease == 2 + sample_groups <- c("Normal", sample_disease_group) + m_prop$Disease <- factor(sample_groups[(m_prop$Disease_factor > phenotype_target_threshold) + 1], # nolint + levels = sample_groups) -## Binary to scale: e.g. TRUE / 5 = 0.2 -m_prop$D <- (m_prop$Disease == # nolint - sample_disease_group) / sample_disease_group_scale -## NA's are not included in the comparison below -m_prop <- rbind(subset(m_prop, Disease != sample_disease_group), - subset(m_prop, Disease == sample_disease_group)) + ## Binary to scale: e.g. TRUE / 5 = 0.2 + m_prop$D <- (m_prop$Disease == # nolint + sample_disease_group) / sample_disease_group_scale + ## NA's are not included in the comparison below + m_prop <- rbind(subset(m_prop, Disease != sample_disease_group), + subset(m_prop, Disease == sample_disease_group)) -jitter_new <- ggplot(m_prop, aes(Method, Prop)) + - geom_point(aes(fill = Method, color = Disease, stroke = D, shape = Disease), - size = 2, alpha = 0.7, - position = position_jitter(width = 0.25, height = 0)) + - facet_wrap(~ CellType, scales = "free") + - scale_colour_manual(values = c("white", "gray20")) + - scale_shape_manual(values = c(21, 24)) + theme_minimal() + jitter_new <- scale_yaxes(ggplot(m_prop, aes(Method, Prop)) + + geom_point(aes(fill = Method, color = Disease, stroke = D, shape = Disease), + size = 2, alpha = 0.7, + position = position_jitter(width = 0.25, height = 0)) + + facet_wrap(~ CellType, scales = "free") + + scale_colour_manual(values = c("white", "gray20")) + + scale_shape_manual(values = c(21, 24)) + theme_minimal(), maxyscale) + +} + +if (use_disease_factor) { -## Plot to compare method effectiveness -## Create dataframe for beta cell proportions and Disease_factor levels -m_prop_ana <- data.frame(pData(bulk_eset)[rep(1:nrow(estimated_music_props), 2), #nolint - phenotype_factors], - ct.prop = c(estimated_music_props[, 2], - estimated_nnls_props[, 2]), - Method = factor(rep(methods, - each = nrow(estimated_music_props)), - levels = methods)) -colnames(m_prop_ana)[1:length(phenotype_factors)] <- phenotype_factors #nolint -m_prop_ana <- subset(m_prop_ana, !is.na(m_prop_ana[phenotype_target])) -m_prop_ana$Disease <- factor(sample_groups[( # nolint - m_prop_ana[phenotype_target] > phenotype_target_threshold) + 1], - sample_groups) -m_prop_ana$D <- (m_prop_ana$Disease == # nolint - sample_disease_group) / sample_disease_group_scale + ## Plot to compare method effectiveness + ## Create dataframe for beta cell proportions and Disease_factor levels + ## - Ugly code. Essentially, doubles the cell type proportions for each + ## set of MuSiC and NNLS methods + m_prop_ana <- data.frame(pData(bulk_eset)[rep(1:nrow(estimated_music_props), 2), #nolint + phenotype_factors], + ## get proportions of target cell type + ct.prop = c(estimated_music_props[, phenotype_scrna_target], + estimated_nnls_props[, phenotype_scrna_target]), + ## + Method = factor(rep(methods, + each = nrow(estimated_music_props)), + levels = methods)) + ## - fix headers + colnames(m_prop_ana)[1:length(phenotype_factors)] <- phenotype_factors #nolint + ## - drop NA for target phenotype (e.g. hba1c) + m_prop_ana <- subset(m_prop_ana, !is.na(m_prop_ana[phenotype_target])) + m_prop_ana$Disease <- factor( # nolint + ## - Here we set Normal/Disease assignments across the two MuSiC and NNLS methods + sample_groups[( + m_prop_ana[phenotype_target] > phenotype_target_threshold) + 1 + ], + sample_groups) + ## - Then we scale this binary assignment to a plotable factor + m_prop_ana$D <- (m_prop_ana$Disease == # nolint + sample_disease_group) / sample_disease_group_scale -jitt_compare <- ggplot(m_prop_ana, aes_string(phenotype_target, "ct.prop")) + - geom_smooth(method = "lm", se = FALSE, col = "black", lwd = 0.25) + - geom_point(aes(fill = Method, color = Disease, stroke = D, shape = Disease), - size = 2, alpha = 0.7) + facet_wrap(~ Method) + - ggtitle(compare_title) + theme_minimal() + - scale_colour_manual(values = c("white", "gray20")) + - scale_shape_manual(values = c(21, 24)) + jitt_compare <- scale_yaxes(ggplot(m_prop_ana, aes_string(phenotype_target, "ct.prop")) + + geom_smooth(method = "lm", se = FALSE, col = "black", lwd = 0.25) + + geom_point(aes(fill = Method, color = Disease, stroke = D, shape = Disease), + size = 2, alpha = 0.7) + facet_wrap(~ Method) + + ggtitle(paste0(toupper(phenotype_target), " vs. ", + toupper(phenotype_scrna_target), " Cell Type Proportion")) + + theme_minimal() + + ylab(paste0("Proportion of ", + phenotype_scrna_target, " cells")) + + xlab(paste0("Level of bulk factor (", phenotype_target, ")")) + + scale_colour_manual(values = c("white", "gray20")) + + scale_shape_manual(values = c(21, 24)), maxyscale) +} ## BoxPlot -plot_box <- Boxplot_Est(list( +plot_box <- scale_yaxes(Boxplot_Est(list( data.matrix(estimated_music_props), data.matrix(estimated_nnls_props)), method.name = c("MuSiC", "NNLS")) + theme(axis.text.x = element_text(angle = -90), axis.text.y = element_text(size = 8)) + - ggtitle(element_blank()) + theme_minimal() + ggtitle(element_blank()) + theme_minimal(), maxyscale) ## Heatmap plot_hmap <- Prop_heat_Est(list( @@ -125,8 +155,15 @@ axis.text.y = element_text(size = 6)) pdf(file = outfile_pdf, width = 8, height = 8) -plot_grid(jitter_fig, plot_box, labels = "auto", ncol = 1, nrow = 2) -plot_grid(jitter_new, jitt_compare, labels = "auto", ncol = 1, nrow = 2) +if (length(celltypes) <= 8) { + plot_grid(jitter_fig, plot_box, labels = "auto", ncol = 1, nrow = 2) +} else { + print(jitter_fig) + plot_box +} +if (use_disease_factor) { + plot_grid(jitter_new, jitt_compare, labels = "auto", ncol = 1, nrow = 2) +} plot_hmap message(dev.off()) @@ -159,29 +196,32 @@ quote = F, sep = "\t", col.names = NA) -## Summary table -for (meth in methods) { - ##lm_beta_meth = lm(ct.prop ~ age + bmi + hba1c + gender, data = - sub_data <- subset(m_prop_ana, Method == meth) - ## We can only do regression where there are more than 1 factors - ## so we must find and exclude the ones which are not - gt1_facts <- sapply(phenotype_factors, function(facname) { - return(length(unique(sort(sub_data[[facname]]))) == 1) - }) - form_factors <- phenotype_factors - exclude_facts <- names(gt1_facts)[gt1_facts] - if (length(exclude_facts) > 0) { - message("Factors with only one level will be excluded:") - message(exclude_facts) - form_factors <- phenotype_factors[ - !(phenotype_factors %in% exclude_facts)] +if (use_disease_factor) { + ## Summary table of linear regressions of disease factors + for (meth in methods) { + ##lm_beta_meth = lm(ct.prop ~ age + bmi + hba1c + gender, data = + sub_data <- subset(m_prop_ana, Method == meth) + + ## We can only do regression where there are more than 1 factors + ## so we must find and exclude the ones which are not + gt1_facts <- sapply(phenotype_factors, function(facname) { + return(length(unique(sort(sub_data[[facname]]))) == 1) + }) + form_factors <- phenotype_factors + exclude_facts <- names(gt1_facts)[gt1_facts] + if (length(exclude_facts) > 0) { + message("Factors with only one level will be excluded:") + message(exclude_facts) + form_factors <- phenotype_factors[ + !(phenotype_factors %in% exclude_facts)] + } + lm_beta_meth <- lm(as.formula( + paste("ct.prop", paste(form_factors, collapse = " + "), + sep = " ~ ")), data = sub_data) + message(paste0("Summary: ", meth)) + capture.output(summary(lm_beta_meth), + file = paste0("report_data/summ_Log of ", + meth, + " fitting.txt")) } - lm_beta_meth <- lm(as.formula( - paste("ct.prop", paste(form_factors, collapse = " + "), - sep = " ~ ")), data = sub_data) - message(paste0("Summary: ", meth)) - capture.output(summary(lm_beta_meth), - file = paste0("report_data/summ_Log of ", - meth, - " fitting.txt")) }
--- a/scripts/inspect.R Fri Nov 26 15:55:11 2021 +0000 +++ /dev/null Thu Jan 01 00:00:00 1970 +0000 @@ -1,27 +0,0 @@ - -suppressWarnings(suppressPackageStartupMessages(library(xbioc))) -suppressWarnings(suppressPackageStartupMessages(library(MuSiC))) - -args <- commandArgs(trailingOnly = TRUE) -source(args[1]) - -printout <- function(text) { - if (typeof(text) %in% c("list", "vector", "integer", "double", "numeric")) { - write.table(text, file = outfile_tab, quote = F, sep = "\t", - col.names = NA) - } else { - ## text - print(typeof(text)) - capture.output(text, file = outfile_tab) # nolint - } -} - -if (inspector %in% c("print", "pData", "fData", "dims", - "experimentData", "protocolData", "exprs", - "signature", "annotation", "abstract")) { - op <- get(inspector) - tab <- op(rds_eset) - printout(tab) -} else { - stop(paste0("No such option:", inspector)) -}
--- /dev/null Thu Jan 01 00:00:00 1970 +0000 +++ b/test-data/mouse_scrna_exprs.tabular Sat Jan 29 12:52:10 2022 +0000 @@ -0,0 +1,101 @@ + TGGTTCCGTCGGCTCA-2 CGAGCCAAGCGTCAAG-4 GAATGAAGTTTGGGCC-5 CTCGTACGTTGCCTCT-7 TTCTCAATCCACGCAG-5 CCTTCCCCATACCATG-4 ACTTTCACAGCTGGCT-7 TGGGAAGCAAAGTGCG-7 TCTATTGAGTAGGCCA-7 TCGGTAACATCACGTA-2 GGGTTGCCAGCTGTAT-2 TGCGGGTGTCATATCG-6 ACTTGTTTCATATCGG-5 CCAATCCCACGGCGTT-2 CTAAGACCACCAGGCT-7 TTAACTCAGTAGGCCA-6 GTACTCCGTAACGCGA-1 GCCTCTAGTTGTACAC-2 TTCGAAGTCCTGCAGG-3 TTCTACAAGTTGTAGA-7 CCGTTCAGTTGAACTC-7 GTGTTAGTCAGCTCGG-1 GGATTACGTGTGCGTC-6 TACGGTATCCGTTGTC-6 TTAGTTCGTATTAGCC-5 CCCAATCGTAGCGATG-3 ACACCAATCTGCGTAA-7 AATCCAGTCCAAACTG-7 CAGAATCAGCAATATG-1 GCACATAAGCCGGTAA-5 CCTTCCCAGGAGTTTA-5 CGGAGCTAGGACTGGT-5 TACGGATGTAAATGTG-4 GGCAATTCATTCACTT-2 CTCGGGAGTCTGCGGT-4 CATTCGCGTCCTCTTG-2 CGCGTTTAGATCGATA-1 GGGTTGCCACCAACCG-4 TGTGTTTCATCGATGT-2 AGAGTGGAGCTGTTCA-7 CTCACACGTCTCACCT-3 AGTTGGTTCCACGAAT-7 ATCTGCCAGACCACGA-6 TGTATTCCATTGAGCT-7 TGAAAGAGTAGCCTAT-7 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--- /dev/null Thu Jan 01 00:00:00 1970 +0000 +++ b/test-data/mouse_scrna_pheno.tabular Sat Jan 29 12:52:10 2022 +0000 @@ -0,0 +1,101 @@ + sampleID SubjectName cellTypeID cellType +TGGTTCCGTCGGCTCA-2 2 Mouse2 3 PT +CGAGCCAAGCGTCAAG-4 4 Mouse4 5 DCT +GAATGAAGTTTGGGCC-5 5 Mouse5 3 PT +CTCGTACGTTGCCTCT-7 7 Mouse7 3 PT +TTCTCAATCCACGCAG-5 5 Mouse5 4 LOH +CCTTCCCCATACCATG-4 4 Mouse4 14 T lymph +ACTTTCACAGCTGGCT-7 7 Mouse7 3 PT +TGGGAAGCAAAGTGCG-7 7 Mouse7 3 PT +TCTATTGAGTAGGCCA-7 7 Mouse7 3 PT +TCGGTAACATCACGTA-2 2 Mouse2 3 PT +GGGTTGCCAGCTGTAT-2 2 Mouse2 2 Podo +TGCGGGTGTCATATCG-6 6 Mouse6 3 PT +ACTTGTTTCATATCGG-5 5 Mouse5 14 T lymph +CCAATCCCACGGCGTT-2 2 Mouse2 5 DCT +CTAAGACCACCAGGCT-7 7 Mouse7 3 PT +TTAACTCAGTAGGCCA-6 6 Mouse6 3 PT +GTACTCCGTAACGCGA-1 1 Mouse1 3 PT +GCCTCTAGTTGTACAC-2 2 Mouse2 3 PT +TTCGAAGTCCTGCAGG-3 3 Mouse3 3 PT +TTCTACAAGTTGTAGA-7 7 Mouse7 3 PT +CCGTTCAGTTGAACTC-7 7 Mouse7 7 CD-IC +GTGTTAGTCAGCTCGG-1 1 Mouse1 4 LOH +GGATTACGTGTGCGTC-6 6 Mouse6 3 PT +TACGGTATCCGTTGTC-6 6 Mouse6 3 PT +TTAGTTCGTATTAGCC-5 5 Mouse5 3 PT +CCCAATCGTAGCGATG-3 3 Mouse3 3 PT +ACACCAATCTGCGTAA-7 7 Mouse7 5 DCT +AATCCAGTCCAAACTG-7 7 Mouse7 5 DCT +CAGAATCAGCAATATG-1 1 Mouse1 3 PT +GCACATAAGCCGGTAA-5 5 Mouse5 5 DCT +CCTTCCCAGGAGTTTA-5 5 Mouse5 3 PT +CGGAGCTAGGACTGGT-5 5 Mouse5 4 LOH +TACGGATGTAAATGTG-4 4 Mouse4 3 PT +GGCAATTCATTCACTT-2 2 Mouse2 3 PT +CTCGGGAGTCTGCGGT-4 4 Mouse4 6 CD-PC +CATTCGCGTCCTCTTG-2 2 Mouse2 8 CD-Trans +CGCGTTTAGATCGATA-1 1 Mouse1 6 CD-PC +GGGTTGCCACCAACCG-4 4 Mouse4 7 CD-IC +TGTGTTTCATCGATGT-2 2 Mouse2 3 PT +AGAGTGGAGCTGTTCA-7 7 Mouse7 3 PT +CTCACACGTCTCACCT-3 3 Mouse3 3 PT +AGTTGGTTCCACGAAT-7 7 Mouse7 3 PT +ATCTGCCAGACCACGA-6 6 Mouse6 3 PT +TGTATTCCATTGAGCT-7 7 Mouse7 3 PT +TGAAAGAGTAGCCTAT-7 7 Mouse7 3 PT +AAATGCCAGAACTGTA-7 7 Mouse7 5 DCT +TTTGCGCTCTACCAGA-4 4 Mouse4 3 PT +ACATACGGTTTCCACC-6 6 Mouse6 3 PT +GCCTCTAGTTCCACAA-7 7 Mouse7 3 PT +GGGAGATGTACTCTCC-6 6 Mouse6 1 Endo +GAACGGATCTTGTACT-7 7 Mouse7 3 PT +TACCTTATCCTAGAAC-1 1 Mouse1 3 PT +GCGCGATAGATGCCAG-2 2 Mouse2 3 PT +GACAGAGCAAGTTGTC-7 7 Mouse7 3 PT +TGACTAGGTATGAATG-3 3 Mouse3 4 LOH +CACACTCAGTCACGCC-6 6 Mouse6 3 PT +ATTGGTGGTTAGGGTG-5 5 Mouse5 3 PT +AGCAGCCCAGCGTAAG-2 2 Mouse2 1 Endo +CATTCGCAGCCTTGAT-6 6 Mouse6 3 PT +GCGAGAACATAGACTC-2 2 Mouse2 14 T lymph +AGTCTTTGTAATAGCA-7 7 Mouse7 3 PT +TCGCGAGCAGACACTT-7 7 Mouse7 3 PT +CGGAGTCCAGCAGTTT-2 2 Mouse2 3 PT +GGTGTTACACACATGT-7 7 Mouse7 3 PT +TTCTCAAGTAAGTGTA-2 2 Mouse2 1 Endo +TGCTGCTAGTCAATAG-2 2 Mouse2 3 PT +GATGAGGTCTACCAGA-2 2 Mouse2 3 PT +ACATACGGTTGTACAC-5 5 Mouse5 3 PT +ACGAGGACAGCTATTG-7 7 Mouse7 4 LOH +CGATGTATCGGCGGTT-2 2 Mouse2 3 PT +CTGCGGATCACAACGT-2 2 Mouse2 13 B lymph +CGAACATAGTTGAGTA-5 5 Mouse5 3 PT +TAGTTGGTCGCGATCG-6 6 Mouse6 5 DCT +GCAGCCACAATGTAAG-4 4 Mouse4 1 Endo +CTCACACCAATAACGA-7 7 Mouse7 3 PT +CCTTTCTCATGAAGTA-2 2 Mouse2 7 CD-IC +AGTGTCAAGAGCAATT-7 7 Mouse7 3 PT +AGCATACGTAAAGGAG-1 1 Mouse1 6 CD-PC +ACACCAATCTCGCTTG-5 5 Mouse5 3 PT +GGGATGAGTATCAGTC-6 6 Mouse6 3 PT +TGACAACAGAAGCCCA-2 2 Mouse2 3 PT +CGAATGTTCACAATGC-1 1 Mouse1 1 Endo +GCACTCTTCCGCATAA-1 1 Mouse1 3 PT +CACCAGGTCCCAAGAT-2 2 Mouse2 3 PT +GTTACAGCACCGCTAG-6 6 Mouse6 3 PT +TAGCCGGCAGTACACT-2 2 Mouse2 11 Macro +ACGATGTGTTAAAGAC-2 2 Mouse2 9 Novel1 +CCTTCCCAGTCTCGGC-7 7 Mouse7 3 PT +TAGTGGTTCTCTGTCG-7 7 Mouse7 7 CD-IC +TAGCCGGAGGCTAGCA-5 5 Mouse5 7 CD-IC +TTGTAGGTCAGCACAT-1 1 Mouse1 4 LOH +GAATAAGCAGCTTCGG-7 7 Mouse7 3 PT +TCGCGAGAGTCCGGTC-3 3 Mouse3 14 T lymph +TCAACGAAGAGTAAGG-2 2 Mouse2 5 DCT +CAGGTGCCACGAAATA-5 5 Mouse5 3 PT +TGTGTTTCACTATCTT-2 2 Mouse2 3 PT +TGGCCAGAGTGAAGAG-6 6 Mouse6 3 PT +ACCAGTAAGTAGCCGA-2 2 Mouse2 6 CD-PC +GCGGGTTAGAAGGTTT-1 1 Mouse1 3 PT +CAGTCCTGTCATTAGC-2 2 Mouse2 7 CD-IC