Last updated: 2022-02-24
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Knit directory: scATACseq-topics/
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Modified: scripts/fit_all_models_Cusanovich2018.sh
Modified: scripts/postfit_Buenrostro2018_Chen2019pipeline.sh
Modified: scripts/postfit_Cusanovich2018.sh
Modified: scripts/postfit_gene_analysis.sbatch
Note that any generated files, e.g. HTML, png, CSS, etc., are not included in this status report because it is ok for generated content to have uncommitted changes.
These are the previous versions of the repository in which changes were made to the R Markdown (analysis/motif_analysis_Buenrostro2018_Chen2019pipeline_v2.Rmd
) and HTML (docs/motif_analysis_Buenrostro2018_Chen2019pipeline_v2.html
) files. If you've configured a remote Git repository (see ?wflow_git_remote
), click on the hyperlinks in the table below to view the files as they were in that past version.
File | Version | Author | Date | Message |
---|---|---|---|---|
Rmd | 2bd895b | kevinlkx | 2022-02-24 | wflow_publish("analysis/motif_analysis_Buenrostro2018_Chen2019pipeline_v2.Rmd") |
html | 5c83f24 | kevinlkx | 2022-02-16 | Build site. |
Rmd | c1e1d7e | kevinlkx | 2022-02-16 | updated with new DA test result |
Here we perform TF motif analysis for the Buenrostro et al (2018) scATAC-seq result inferred from the multinomial topic model with \(k = 11\).
We use binarized scPeaks and scATAC-seq data was processed using Chen et al (2019) pipeline.
library(Matrix)
library(fastTopics)
library(dplyr)
library(tidyr)
library(ggplot2)
library(ggrepel)
library(cowplot)
library(plotly)
library(htmlwidgets)
library(DT)
library(reshape2)
library(Logolas)
library(grid)
source("code/motif_analysis.R")
source("code/plots.R")
Load the binarized data and the \(k = 11\) Poisson NMF fit results
data.dir <- "/project2/mstephens/kevinluo/scATACseq-topics/data/Buenrostro_2018/processed_data_Chen2019pipeline/"
load(file.path(data.dir, "Buenrostro_2018_binarized_counts.RData"))
cat(sprintf("%d x %d counts matrix.\n",nrow(counts),ncol(counts)))
# 2034 x 101172 counts matrix.
fit.dir <- "/project2/mstephens/kevinluo/scATACseq-topics/output/Buenrostro_2018_Chen2019pipeline/binarized/"
fit <- readRDS(file.path(fit.dir, "/fit-Buenrostro2018-binarized-scd-ex-k=11.rds"))$fit
fit <- poisson2multinom(fit)
set.seed(10)
colors_topics <- c("#a6cee3","#1f78b4","#b2df8a","#33a02c","#fb9a99","#e31a1c",
"#fdbf6f","#ff7f00","#cab2d6","#6a3d9a","#ffff99","#b15928",
"gray")
samples$label <- factor(samples$label, levels = c("HSC", "MPP", "CMP", "GMP", "mono", "MEP", "LMPP", "CLP", "pDC", "UNK"))
p.structure <- structure_plot(fit,
grouping = samples[, "label"],n = Inf,gap = 40,
perplexity = 50,colors = colors_topics,
num_threads = 4,verbose = FALSE)
print(p.structure)
Version | Author | Date |
---|---|---|
5c83f24 | kevinlkx | 2022-02-16 |
set.seed(10)
colors_topics <- c("#a6cee3","#1f78b4","#b2df8a","#33a02c","#fb9a99","#e31a1c",
"#fdbf6f","#ff7f00","#cab2d6","#6a3d9a","#ffff99","#b15928",
"gray")
myeloid_samples <- factor(samples$label, levels = c("HSC", "MPP", "CMP", "GMP", "mono"))
p.structure.myeloid <- structure_plot(fit,
grouping = myeloid_samples, n = Inf,gap = 40,
perplexity = 50, colors = colors_topics,
num_threads = 4,verbose = FALSE)
print(p.structure.myeloid)
Version | Author | Date |
---|---|---|
5c83f24 | kevinlkx | 2022-02-16 |
set.seed(10)
colors_topics <- c("#a6cee3","#1f78b4","#b2df8a","#33a02c","#fb9a99","#e31a1c",
"#fdbf6f","#ff7f00","#cab2d6","#6a3d9a","#ffff99","#b15928",
"gray")
myeloid_samples <- factor(samples$label, levels = c("HSC", "MPP", "CMP", "MEP"))
p.structure.erythroid <- structure_plot(fit,
grouping = myeloid_samples, n = Inf,gap = 40,
perplexity = 50,colors = colors_topics,
num_threads = 4,verbose = FALSE)
print(p.structure.erythroid)
Version | Author | Date |
---|---|---|
5c83f24 | kevinlkx | 2022-02-16 |
set.seed(10)
colors_topics <- c("#a6cee3","#1f78b4","#b2df8a","#33a02c","#fb9a99","#e31a1c",
"#fdbf6f","#ff7f00","#cab2d6","#6a3d9a","#ffff99","#b15928",
"gray")
myeloid_samples <- factor(samples$label, levels = c("HSC", "MPP", "LMPP", "CLP"))
p.structure.lymphoid <- structure_plot(fit,
grouping = myeloid_samples, n = Inf,gap = 40,
perplexity = 50,colors = colors_topics,
num_threads = 4,verbose = FALSE)
print(p.structure.lymphoid)
Version | Author | Date |
---|---|---|
5c83f24 | kevinlkx | 2022-02-16 |
Load results from differential accessbility analysis for the topics
out.dir <- "/project2/mstephens/kevinluo/scATACseq-topics/output/Buenrostro_2018_Chen2019pipeline/binarized/postfit_v2"
cat(sprintf("Load results from %s \n", out.dir))
DA_res <- readRDS(file.path(out.dir, paste0("DAanalysis-Buenrostro2018-k=11/DA_regions_topics_10000iters.rds")))
# Load results from /project2/mstephens/kevinluo/scATACseq-topics/output/Buenrostro_2018_Chen2019pipeline/binarized/postfit_v2
Volcano plot of the regions
topic 1 and topic 4 examples
p.volcano.1 <- volcano_plot(DA_res,k = 1, labels = rep("",nrow(DA_res$z)))
p.volcano.4 <- volcano_plot(DA_res,k = 4, labels = rep("",nrow(DA_res$z)))
plot_grid(p.volcano.1, p.volcano.4)
Version | Author | Date |
---|---|---|
5c83f24 | kevinlkx | 2022-02-16 |
all topics
plots <- vector("list",11)
names(plots) <- 1:11
for (k in 1:11)
plots[[k]] <- volcano_plot(DA_res, k, labels = rep("",nrow(DA_res$z)))
do.call(plot_grid,plots)
Compile Homer results across topics
homer.dir <- paste0(out.dir, "/motifanalysis-Buenrostro2018-k=11-quantile/HOMER/")
cat(sprintf("Directory of motif analysis result: %s \n", homer.dir))
homer_res_topics <- readRDS(file.path(homer.dir, "/homer_knownResults.rds"))
selected_regions <- readRDS(file.path(homer.dir, "/selected_regions.rds"))
# Compile Homer results (pvalue and ranking) across topics
motif_res <- compile_homer_motif_res(homer_res_topics)
saveRDS(motif_res, paste0(homer.dir, "/homer_motif_enrichment_results.rds"))
cat("compiled homer motif results are saved in", paste0(homer.dir, "/homer_motif_enrichment_results.rds \n"))
motif_table <- data.frame(motif = gsub("/.*", "", rownames(motif_res$mlog10P)),
round(motif_res$mlog10P,2))
DT::datatable(motif_table, rownames = F, caption = "Motif enrichment (-log10P)")
# Directory of motif analysis result: /project2/mstephens/kevinluo/scATACseq-topics/output/Buenrostro_2018_Chen2019pipeline/binarized/postfit_v2/motifanalysis-Buenrostro2018-k=11-quantile/HOMER/
# compiled homer motif results are saved in /project2/mstephens/kevinluo/scATACseq-topics/output/Buenrostro_2018_Chen2019pipeline/binarized/postfit_v2/motifanalysis-Buenrostro2018-k=11-quantile/HOMER//homer_motif_enrichment_results.rds
cat("Number of regions selected for each topic: \n")
print(mapply(nrow, selected_regions[1:(length(selected_regions)-1)]))
colnames_homer <- c("motif_name", "consensus", "P", "log10P", "Padj", "num_target", "percent_target", "num_bg", "percent_bg")
top_motifs <- data.frame(matrix(nrow=10, ncol = length(homer_res_topics)))
colnames(top_motifs) <- names(homer_res_topics)
for (k in 1:length(homer_res_topics)){
homer_res <- homer_res_topics[[k]]
colnames(homer_res) <- colnames_homer
homer_res <- homer_res %>% separate(motif_name, c("motif", "origin", "database"), "/")
top_motifs[,k] <- head(homer_res$motif, 10)
}
DT::datatable(data.frame(rank = 1:10, top_motifs), rownames = F, caption = "Top 10 motifs enriched in each topic.")
# Number of regions selected for each topic:
# k1 k2 k3 k4 k5 k6 k7 k8 k9 k10 k11
# 1012 1012 1012 1012 1012 1012 1012 1012 1012 1012 1012
Heatmap of motif enrichment -log10(p-value).
create_motif_enrichment_heatmap(motif_res, enrichment = "-log10(p-value)",
cluster_motifs = TRUE, cluster_topics = TRUE, motif_filter = 10, horizontal = FALSE,
enrichment_range = c(0,100), method_cluster = "average", font.size.motifs = 4, font.size.topics = 9)
Version | Author | Date |
---|---|---|
5c83f24 | kevinlkx | 2022-02-16 |
# 137 out of 439 motifs included the heatmap
# Heatmap of motif enrichment z-score.
create_motif_enrichment_heatmap(motif_res, enrichment = "z-score",
cluster_motifs = TRUE, cluster_topics = FALSE, motif_filter = 10, horizontal = FALSE,
enrichment_range = c(-20,20), method_cluster = "average", font.size.motifs = 4, font.size.topics = 9)
toMatch <- c("^GATA\\d*$", "^CEBP.?$", "^SPI.?$", "^IRF\\d*$", "^STAT\\d*$", "^TCF\\d*$", "^BCL\\d*$", "^CTCF$", "^ERG$")
selected_motifs <- grep(paste(toMatch,collapse="|"), motif_res$motifs$motif, ignore.case = T, value = T)
rows <- match(selected_motifs, motif_res$motifs$motif)
selected_motif_res <- lapply(motif_res, FUN = function(x) {x[rows, ]})
Heatmap of motif enrichment -log10(p-value). Order motifs by hierarchical clustering.
create_motif_enrichment_heatmap(selected_motif_res, enrichment = "-log10(p-value)",
cluster_motifs = TRUE, cluster_topics = TRUE, motif_filter = 10, horizontal = FALSE,
enrichment_range = c(0,100), method_cluster = "average", font.size.motifs = 8, font.size.topics = 9)
Version | Author | Date |
---|---|---|
5c83f24 | kevinlkx | 2022-02-16 |
# 17 out of 26 motifs included the heatmap
Plot motif enrichment (-log10 p-value) and the ranking
# Plot enrichment (-log10 p-value) and ranking of the motifs
plots <- vector("list", ncol(motif_res$mlog10P))
names(plots) <- colnames(motif_res$mlog10P)
for( i in 1:length(plots)){
plots[[i]] <- create_motif_enrichment_ranking_plot(motif_res, k = i,
max.overlaps = 20, subsample = FALSE)
}
do.call(plot_grid,plots)
Version | Author | Date |
---|---|---|
5c83f24 | kevinlkx | 2022-02-16 |
Examples Topic 1 is mainly shown in GMP. The enrichment of CEBP motif in GMP is also highlighted in Figure 2F of the Buenrostro et al paper.
Topic 4 is mainly shown in MEP especially and also CMP. The enrichment of GATA motif in MEP and CMP is also highlighted in Figure 2E of the Buenrostro et al paper.
do.call(plot_grid,plots[c(1,4)])
Version | Author | Date |
---|---|---|
5c83f24 | kevinlkx | 2022-02-16 |
# Plot motif enrichment (-log10 p-value) in each topic vs other topics
plots <- vector("list", ncol(motif_res$mlog10P))
names(plots) <- colnames(motif_res$mlog10P)
for( i in 1:length(homer_res_topics)){
plots[[i]] <- create_motif_enrichment_plot(motif_res, k = i,
max.overlaps = 20, subsample = TRUE)
}
do.call(plot_grid,plots)
Load pre-computed gene scores
Gene scores were computed using TSS based method as in Lareau et al Nature Biotech, 2019 as well as the model 21
in archR
paper. This model weights chromatin accessibility around gene promoters by using bi-directional exponential decays from the TSS.
gene.dir <- paste0(out.dir, "/geneanalysis-Buenrostro2018-k=11-TSS-absZ-l2")
cat(sprintf("Directory of gene analysis result: %s \n", gene.dir))
genescore_res <- readRDS(file.path(gene.dir, "genescore_result.rds"))
# Directory of gene analysis result: /project2/mstephens/kevinluo/scATACseq-topics/output/Buenrostro_2018_Chen2019pipeline/binarized/postfit_v2/geneanalysis-Buenrostro2018-k=11-TSS-absZ-l2
Get TF genes
motif_names <- motif_res$motifs$motif
gene_names <- genescore_res$genes$SYMBOL
common_genes <- intersect(toupper(motif_names), toupper(gene_names))
cat(sprintf("%s TF genes mapped between motif names and gene symbol. \n", length(common_genes)))
motif_gene_table <- data.frame(motif = motif_names[match(common_genes, toupper(motif_names))],
gene = gene_names[match(common_genes, toupper(gene_names))])
# 263 TF genes mapped between motif names and gene symbol.
Compute correlation between motif enrichment z-score and gene score:
Topic 4 example
motif_gene_mapping <- create_motif_gene_cor_scatterplot(motif_res, genescore_res, motif_gene_table,
k = 4, cor.motif = "z-score")
Version | Author | Date |
---|---|---|
5c83f24 | kevinlkx | 2022-02-16 |
motif_gene_mapping <- motif_gene_mapping[with(motif_gene_mapping, order(motif_mlog10P*cor_zscore, decreasing = T)),]
rownames(motif_gene_mapping) <- 1:nrow(motif_gene_mapping)
cat("Top 10 motifs by motif enrichment (-log10 p-value) and correlation to gene scores: \n")
print(head(motif_gene_mapping[,c("motif","motif_mlog10P", "gene_score", "cor_zscore")], 10))
# Top 10 motifs by motif enrichment (-log10 p-value) and correlation to gene scores:
# motif motif_mlog10P gene_score cor_zscore
# 1 Gata1(Zf) 221.490186 0.093355787 0.8026633
# 2 Gata6(Zf) 272.042063 0.014304687 0.1222153
# 3 Sp2(Zf) 8.846579 0.009008670 0.8859293
# 4 Klf4(Zf) 7.808615 0.018467354 0.7009582
# 5 MYB(HTH) 12.451223 0.033500629 0.3270266
# 6 KLF6(Zf) 10.540327 0.007717778 0.3080052
# 7 Twist2(bHLH) 8.764063 0.002548089 0.3316900
# 8 KLF3(Zf) 4.798954 0.046606706 0.5499308
# 9 KLF1(Zf) 8.277653 0.292057556 0.2978747
# 10 Maz(Zf) 2.858961 0.003280518 0.7933922
GATA family
motif_names <- motif_res$motifs$motif
gene_names <- genescore_res$genes$SYMBOL
TF_motifs <- sort(unique(grep("^GATA\\d*$", motif_names, ignore.case=T, value=T)))
TF_genes <- sort(unique(grep("^GATA\\d*$", gene_names, ignore.case=T, value=T)))
common_genes <- intersect(toupper(TF_motifs), toupper(TF_genes))
motif_gene_table <- data.frame(motif = TF_motifs[match(common_genes, toupper(TF_motifs))],
gene = TF_genes[match(common_genes, toupper(TF_genes))])
print(motif_gene_table)
# motif gene
# 1 Gata1 GATA1
# 2 Gata2 GATA2
# 3 GATA3 GATA3
# 4 Gata4 GATA4
# 5 Gata6 GATA6
# Plot GATA motifs in topic 4
k = 4
motif_order <- order(motif_res$mlog10P[,k], decreasing = T)
motifs <- rownames(motif_res$motifs[motif_order,])
motif_names <- motif_res$motifs[motif_order, "motif"]
selected_motifs <- unique(motifs[match(toupper(motif_gene_table$motif), toupper(motif_names))])
motif.dir <- paste0(homer.dir, "/homer_result_topic_", k, "/knownResults/")
for (i in 1:length(selected_motifs)){
plot_motif_logo(homer_res_topics, selected_motifs[i], k, motif.dir, type = "both")
}
plots <- create_motif_gene_scatterplot(motif_res, genescore_res,
motif_gene_table,
k = 4,
y = "-log10(p-value)",
colors = colors_topics,
max.overlaps = 10)
do.call(plot_grid,plots)
Version | Author | Date |
---|---|---|
5c83f24 | kevinlkx | 2022-02-16 |
plots <- create_motif_gene_scatterplot(motif_res, genescore_res,
motif_gene_table,
k = 4,
y = "z-score",
colors = colors_topics,
max.overlaps = 10)
do.call(plot_grid,plots)
Version | Author | Date |
---|---|---|
5c83f24 | kevinlkx | 2022-02-16 |
CEBP family
motif_names <- motif_res$motifs$motif
gene_names <- genescore_res$genes$SYMBOL
TF_motifs <- sort(unique(grep("^CEBP.?$", motif_names, ignore.case=T, value=T)))
TF_genes <- sort(unique(grep("^CEBP.?$", gene_names, ignore.case=T, value=T)))
motif_gene_table <- unique(data.frame(motif = c("CEBP"), gene = TF_genes))
print(motif_gene_table)
# motif gene
# 1 CEBP CEBPA
# 2 CEBP CEBPB
# 3 CEBP CEBPD
# 4 CEBP CEBPE
# 5 CEBP CEBPG
# 6 CEBP CEBPZ
# Plot GATA motifs in topic 4
k = 1
motif_order <- order(motif_res$mlog10P[,k], decreasing = T)
motifs <- rownames(motif_res$motifs[motif_order,])
motif_names <- motif_res$motifs[motif_order, "motif"]
selected_motifs <- unique(motifs[match(toupper(motif_gene_table$motif), toupper(motif_names))])
motif.dir <- paste0(homer.dir, "/homer_result_topic_", k, "/knownResults/")
for (i in 1:length(selected_motifs)){
plot_motif_logo(homer_res_topics, selected_motifs[i], k, motif.dir, type = "both")
}
plots <- create_motif_gene_scatterplot(motif_res, genescore_res,
motif_gene_table,
k = 1,
y = "-log10(p-value)",
colors = colors_topics,
max.overlaps = 10)
do.call(plot_grid,plots)
Version | Author | Date |
---|---|---|
5c83f24 | kevinlkx | 2022-02-16 |
plots <- create_motif_gene_scatterplot(motif_res, genescore_res,
motif_gene_table,
k = 1,
y = "z-score",
colors = colors_topics,
max.overlaps = 10)
do.call(plot_grid,plots)
Version | Author | Date |
---|---|---|
5c83f24 | kevinlkx | 2022-02-16 |
gene.dir <- paste0(out.dir, "/geneanalysis-Buenrostro2018-k=11-TSS-Z-l2")
cat(sprintf("Directory of gene analysis result: %s \n", gene.dir))
genescore_res <- readRDS(file.path(gene.dir, "genescore_result.rds"))
# Directory of gene analysis result: /project2/mstephens/kevinluo/scATACseq-topics/output/Buenrostro_2018_Chen2019pipeline/binarized/postfit_v2/geneanalysis-Buenrostro2018-k=11-TSS-Z-l2
Get TF genes
motif_names <- motif_res$motifs$motif
gene_names <- genescore_res$genes$SYMBOL
common_genes <- intersect(toupper(motif_names), toupper(gene_names))
cat(sprintf("%s TF genes mapped between motif names and gene symbol. \n", length(common_genes)))
motif_gene_table <- data.frame(motif = motif_names[match(common_genes, toupper(motif_names))],
gene = gene_names[match(common_genes, toupper(gene_names))])
# 263 TF genes mapped between motif names and gene symbol.
Compute correlation between motif enrichment z-score and gene score:
Topic 4 example
motif_gene_mapping <- create_motif_gene_cor_scatterplot(motif_res, genescore_res, motif_gene_table,
k = 4, cor.motif = "z-score")
motif_gene_mapping <- motif_gene_mapping[with(motif_gene_mapping, order(motif_mlog10P*cor_zscore, decreasing = T)),]
rownames(motif_gene_mapping) <- 1:nrow(motif_gene_mapping)
cat("Top 10 motifs by motif enrichment (-log10 p-value) and correlation to gene scores: \n")
print(head(motif_gene_mapping[,c("motif","motif_mlog10P", "gene_score", "cor_zscore")], 10))
# Top 10 motifs by motif enrichment (-log10 p-value) and correlation to gene scores:
# motif motif_mlog10P gene_score cor_zscore
# 1 Gata1(Zf) 221.490186 0.093328287 0.80183826
# 2 Gata2(Zf) 228.178321 0.002122747 0.57764210
# 3 Gata6(Zf) 272.042063 0.008075553 0.46123697
# 4 GATA3(Zf) 262.531014 -0.005200778 0.15806341
# 5 Sp2(Zf) 8.846579 -0.001492563 0.88709250
# 6 RUNX2(Runt) 19.981889 -0.004501222 0.36587553
# 7 MYB(HTH) 12.451223 0.020132756 0.48045456
# 8 TRPS1(Zf) 246.852984 -0.001673225 0.01432698
# 9 TCF4(bHLH) 10.279750 -0.011726683 0.29210084
# 10 Atoh1(bHLH) 8.525201 -0.006685703 0.32340760
GATA family
motif_names <- motif_res$motifs$motif
gene_names <- genescore_res$genes$SYMBOL
TF_motifs <- sort(unique(grep("^GATA\\d*$", motif_names, ignore.case=T, value=T)))
TF_genes <- sort(unique(grep("^GATA\\d*$", gene_names, ignore.case=T, value=T)))
common_genes <- intersect(toupper(TF_motifs), toupper(TF_genes))
motif_gene_table <- data.frame(motif = TF_motifs[match(common_genes, toupper(TF_motifs))],
gene = TF_genes[match(common_genes, toupper(TF_genes))])
print(motif_gene_table)
# motif gene
# 1 Gata1 GATA1
# 2 Gata2 GATA2
# 3 GATA3 GATA3
# 4 Gata4 GATA4
# 5 Gata6 GATA6
plots <- create_motif_gene_scatterplot(motif_res, genescore_res,
motif_gene_table,
k = 4,
y = "-log10(p-value)",
colors = colors_topics,
max.overlaps = 10)
do.call(plot_grid,plots)
plots <- create_motif_gene_scatterplot(motif_res, genescore_res,
motif_gene_table,
k = 4,
y = "z-score",
colors = colors_topics,
max.overlaps = 10)
do.call(plot_grid,plots)
CEBP family
motif_names <- motif_res$motifs$motif
gene_names <- genescore_res$genes$SYMBOL
TF_motifs <- sort(unique(grep("^CEBP.?$", motif_names, ignore.case=T, value=T)))
TF_genes <- sort(unique(grep("^CEBP.?$", gene_names, ignore.case=T, value=T)))
motif_gene_table <- unique(data.frame(motif = c("CEBP"), gene = TF_genes))
print(motif_gene_table)
# motif gene
# 1 CEBP CEBPA
# 2 CEBP CEBPB
# 3 CEBP CEBPD
# 4 CEBP CEBPE
# 5 CEBP CEBPG
# 6 CEBP CEBPZ
plots <- create_motif_gene_scatterplot(motif_res, genescore_res,
motif_gene_table,
k = 1,
y = "-log10(p-value)",
colors = colors_topics,
max.overlaps = 10)
do.call(plot_grid,plots)
plots <- create_motif_gene_scatterplot(motif_res, genescore_res,
motif_gene_table,
k = 1,
y = "z-score",
colors = colors_topics,
max.overlaps = 10)
do.call(plot_grid,plots)
gene.dir <- paste0(out.dir, "/geneanalysis-Buenrostro2018-k=11-TSS-Z-sum")
cat(sprintf("Directory of gene analysis result: %s \n", gene.dir))
genescore_res <- readRDS(file.path(gene.dir, "genescore_result.rds"))
# Directory of gene analysis result: /project2/mstephens/kevinluo/scATACseq-topics/output/Buenrostro_2018_Chen2019pipeline/binarized/postfit_v2/geneanalysis-Buenrostro2018-k=11-TSS-Z-sum
Get TF genes
motif_names <- motif_res$motifs$motif
gene_names <- genescore_res$genes$SYMBOL
common_genes <- intersect(toupper(motif_names), toupper(gene_names))
cat(sprintf("%s TF genes mapped between motif names and gene symbol. \n", length(common_genes)))
motif_gene_table <- data.frame(motif = motif_names[match(common_genes, toupper(motif_names))],
gene = gene_names[match(common_genes, toupper(gene_names))])
# 263 TF genes mapped between motif names and gene symbol.
Compute correlation between motif enrichment z-score and gene score:
GATA family
motif_names <- motif_res$motifs$motif
gene_names <- genescore_res$genes$SYMBOL
TF_motifs <- sort(unique(grep("^GATA\\d*$", motif_names, ignore.case=T, value=T)))
TF_genes <- sort(unique(grep("^GATA\\d*$", gene_names, ignore.case=T, value=T)))
common_genes <- intersect(toupper(TF_motifs), toupper(TF_genes))
motif_gene_table <- data.frame(motif = TF_motifs[match(common_genes, toupper(TF_motifs))],
gene = TF_genes[match(common_genes, toupper(TF_genes))])
print(motif_gene_table)
# motif gene
# 1 Gata1 GATA1
# 2 Gata2 GATA2
# 3 GATA3 GATA3
# 4 Gata4 GATA4
# 5 Gata6 GATA6
plots <- create_motif_gene_scatterplot(motif_res, genescore_res,
motif_gene_table,
k = 4,
y = "z-score",
colors = colors_topics,
max.overlaps = 10)
do.call(plot_grid,plots)
CEBP family
motif_names <- motif_res$motifs$motif
gene_names <- genescore_res$genes$SYMBOL
TF_motifs <- sort(unique(grep("^CEBP.?$", motif_names, ignore.case=T, value=T)))
TF_genes <- sort(unique(grep("^CEBP.?$", gene_names, ignore.case=T, value=T)))
motif_gene_table <- unique(data.frame(motif = c("CEBP"), gene = TF_genes))
print(motif_gene_table)
# motif gene
# 1 CEBP CEBPA
# 2 CEBP CEBPB
# 3 CEBP CEBPD
# 4 CEBP CEBPE
# 5 CEBP CEBPG
# 6 CEBP CEBPZ
plots <- create_motif_gene_scatterplot(motif_res, genescore_res,
motif_gene_table,
k = 1,
y = "z-score",
colors = colors_topics,
max.overlaps = 10)
do.call(plot_grid,plots)
gene.dir <- paste0(out.dir, "/geneanalysis-Buenrostro2018-k=11-genebody-Z-sum")
cat(sprintf("Directory of gene analysis result: %s \n", gene.dir))
genescore_res <- readRDS(file.path(gene.dir, "genescore_result.rds"))
# Directory of gene analysis result: /project2/mstephens/kevinluo/scATACseq-topics/output/Buenrostro_2018_Chen2019pipeline/binarized/postfit_v2/geneanalysis-Buenrostro2018-k=11-genebody-Z-sum
Get TF genes
motif_names <- motif_res$motifs$motif
gene_names <- genescore_res$genes$SYMBOL
common_genes <- intersect(toupper(motif_names), toupper(gene_names))
cat(sprintf("%s TF genes mapped between motif names and gene symbol. \n", length(common_genes)))
motif_gene_table <- data.frame(motif = motif_names[match(common_genes, toupper(motif_names))],
gene = gene_names[match(common_genes, toupper(gene_names))])
# 263 TF genes mapped between motif names and gene symbol.
Compute correlation between motif enrichment z-score and gene score:
GATA family
motif_names <- motif_res$motifs$motif
gene_names <- genescore_res$genes$SYMBOL
TF_motifs <- sort(unique(grep("^GATA\\d*$", motif_names, ignore.case=T, value=T)))
TF_genes <- sort(unique(grep("^GATA\\d*$", gene_names, ignore.case=T, value=T)))
common_genes <- intersect(toupper(TF_motifs), toupper(TF_genes))
motif_gene_table <- data.frame(motif = TF_motifs[match(common_genes, toupper(TF_motifs))],
gene = TF_genes[match(common_genes, toupper(TF_genes))])
print(motif_gene_table)
# motif gene
# 1 Gata1 GATA1
# 2 Gata2 GATA2
# 3 GATA3 GATA3
# 4 Gata4 GATA4
# 5 Gata6 GATA6
plots <- create_motif_gene_scatterplot(motif_res, genescore_res,
motif_gene_table,
k = 4,
y = "z-score",
colors = colors_topics,
max.overlaps = 10)
do.call(plot_grid,plots)
CEBP family
motif_names <- motif_res$motifs$motif
gene_names <- genescore_res$genes$SYMBOL
TF_motifs <- sort(unique(grep("^CEBP.?$", motif_names, ignore.case=T, value=T)))
TF_genes <- sort(unique(grep("^CEBP.?$", gene_names, ignore.case=T, value=T)))
motif_gene_table <- unique(data.frame(motif = c("CEBP"), gene = TF_genes))
print(motif_gene_table)
# motif gene
# 1 CEBP CEBPA
# 2 CEBP CEBPB
# 3 CEBP CEBPD
# 4 CEBP CEBPE
# 5 CEBP CEBPG
# 6 CEBP CEBPZ
plots <- create_motif_gene_scatterplot(motif_res, genescore_res,
motif_gene_table,
k = 1,
y = "z-score",
colors = colors_topics,
max.overlaps = 10)
do.call(plot_grid,plots)
sessionInfo()
# R version 4.0.4 (2021-02-15)
# Platform: x86_64-pc-linux-gnu (64-bit)
# Running under: Scientific Linux 7.4 (Nitrogen)
#
# Matrix products: default
# BLAS/LAPACK: /software/openblas-0.3.13-el7-x86_64/lib/libopenblas_haswellp-r0.3.13.so
#
# locale:
# [1] LC_CTYPE=en_US.UTF-8 LC_NUMERIC=C
# [3] LC_TIME=en_US.UTF-8 LC_COLLATE=en_US.UTF-8
# [5] LC_MONETARY=en_US.UTF-8 LC_MESSAGES=en_US.UTF-8
# [7] LC_PAPER=en_US.UTF-8 LC_NAME=C
# [9] LC_ADDRESS=C LC_TELEPHONE=C
# [11] LC_MEASUREMENT=en_US.UTF-8 LC_IDENTIFICATION=C
#
# attached base packages:
# [1] grid stats graphics grDevices utils datasets methods
# [8] base
#
# other attached packages:
# [1] Logolas_1.3.1 reshape2_1.4.4 DT_0.20 htmlwidgets_1.5.4
# [5] plotly_4.10.0 cowplot_1.1.1 ggrepel_0.9.1 ggplot2_3.3.5
# [9] tidyr_1.1.4 dplyr_1.0.8 fastTopics_0.6-97 Matrix_1.4-0
# [13] workflowr_1.7.0
#
# loaded via a namespace (and not attached):
# [1] Rtsne_0.15 colorspace_2.0-3 seqinr_4.2-8
# [4] ellipsis_0.3.2 class_7.3-20 rprojroot_2.0.2
# [7] fs_1.5.2 rstudioapi_0.13 farver_2.1.0
# [10] listenv_0.8.0 MatrixModels_0.5-0 bit64_4.0.5
# [13] prodlim_2019.11.13 fansi_1.0.2 lubridate_1.8.0
# [16] codetools_0.2-18 splines_4.0.4 knitr_1.37
# [19] ade4_1.7-18 jsonlite_1.7.3 pROC_1.18.0
# [22] mcmc_0.9-7 caret_6.0-90 gridBase_0.4-7
# [25] Rmpfr_0.8-7 ashr_2.2-47 uwot_0.1.11
# [28] compiler_4.0.4 httr_1.4.2 assertthat_0.2.1
# [31] fastmap_1.1.0 lazyeval_0.2.2 cli_3.2.0
# [34] later_1.3.0 prettyunits_1.1.1 htmltools_0.5.2
# [37] quantreg_5.86 tools_4.0.4 gmp_0.6-2.1
# [40] coda_0.19-4 gtable_0.3.0 glue_1.6.2
# [43] Rcpp_1.0.8 jquerylib_0.1.4 vctrs_0.3.8
# [46] ape_5.6-1 nlme_3.1-155 conquer_1.2.1
# [49] crosstalk_1.2.0 iterators_1.0.13 timeDate_3043.102
# [52] CVXR_1.0-10 gower_0.2.2 xfun_0.29
# [55] stringr_1.4.0 globals_0.14.0 ps_1.6.0
# [58] lifecycle_1.0.1 irlba_2.3.5 future_1.23.0
# [61] getPass_0.2-2 MASS_7.3-55 scales_1.1.1
# [64] ipred_0.9-12 hms_1.1.1 promises_1.2.0.1
# [67] parallel_4.0.4 SparseM_1.81 yaml_2.2.2
# [70] pbapply_1.5-0 sass_0.4.0 rpart_4.1-15
# [73] stringi_1.7.6 SQUAREM_2021.1 highr_0.9
# [76] foreach_1.5.1 lava_1.6.10 truncnorm_1.0-8
# [79] rlang_1.0.1 pkgconfig_2.0.3 matrixStats_0.61.0
# [82] evaluate_0.14 lattice_0.20-45 invgamma_1.1
# [85] purrr_0.3.4 labeling_0.4.2 recipes_0.1.17
# [88] bit_4.0.4 processx_3.5.2 tidyselect_1.1.2
# [91] parallelly_1.30.0 plyr_1.8.6 magrittr_2.0.2
# [94] R6_2.5.1 generics_0.1.2 DBI_1.1.2
# [97] pillar_1.7.0 whisker_0.4 withr_2.4.3
# [100] survival_3.2-13 mixsqp_0.3-43 nnet_7.3-17
# [103] tibble_3.1.6 future.apply_1.8.1 crayon_1.5.0
# [106] utf8_1.2.2 rmarkdown_2.11 progress_1.2.2
# [109] data.table_1.14.2 callr_3.7.0 git2r_0.29.0
# [112] ModelMetrics_1.2.2.2 digest_0.6.29 httpuv_1.6.5
# [115] MCMCpack_1.6-0 RcppParallel_5.1.5 stats4_4.0.4
# [118] munsell_0.5.0 viridisLite_0.4.0 bslib_0.3.1
# [121] quadprog_1.5-8