301 lines
10 KiB
R
301 lines
10 KiB
R
#!/usr/bin/env Rscript
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#########################################################
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# TASK: producing boxplots for dr and other muts
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#########################################################
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#=======================================================================
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# working dir and loading libraries
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getwd()
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setwd("~/git/LSHTM_analysis/scripts/plotting")
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getwd()
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#source("Header_TT.R")
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library(ggplot2)
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library(data.table)
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library(dplyr)
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source("combining_dfs_plotting.R")
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rm(merged_df2, merged_df2_comp, merged_df2_lig, merged_df2_comp_lig
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, merged_df3_comp, merged_df3_comp_lig
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, my_df_u, my_df_u_lig)
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cols_to_select = c("mutation", "mutationinformation"
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, "wild_type", "position", "mutant_type"
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, "mutation_info")
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merged_df3_short = merged_df3[, cols_to_select]
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# write merged_df3 to generate structural figure
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write.csv(merged_df3_short, "merged_df3_short.csv")
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#========================================================================
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#%%%%%%%%%%%%%%%%%%%
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# REASSIGNMENT: PS
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#%%%%%%%%%%%%%%%%%%%%
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df_ps = merged_df3
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#============================
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# adding foldx scaled values
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# scale data b/w -1 and 1
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#============================
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n = which(colnames(df_ps) == "ddg"); n
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my_min = min(df_ps[,n]); my_min
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my_max = max(df_ps[,n]); my_max
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df_ps$foldx_scaled = ifelse(df_ps[,n] < 0
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, df_ps[,n]/abs(my_min)
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, df_ps[,n]/my_max)
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# sanity check
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my_min = min(df_ps$foldx_scaled); my_min
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my_max = max(df_ps$foldx_scaled); my_max
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if (my_min == -1 && my_max == 1){
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cat("PASS: foldx ddg successfully scaled b/w -1 and 1"
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, "\nProceeding with assigning foldx outcome category")
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}else{
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cat("FAIL: could not scale foldx ddg values"
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, "Aborting!")
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}
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#================================
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# adding foldx outcome category
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# ddg<0 = "Stabilising" (-ve)
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#=================================
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c1 = table(df_ps$ddg < 0)
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df_ps$foldx_outcome = ifelse(df_ps$ddg < 0, "Stabilising", "Destabilising")
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c2 = table(df_ps$ddg < 0)
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if ( all(c1 == c2) ){
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cat("PASS: foldx outcome successfully created")
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}else{
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cat("FAIL: foldx outcome could not be created. Aborting!")
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exit()
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}
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# name tidying
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df_ps$mutation_info = as.factor(df_ps$mutation_info)
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df_ps$duet_outcome = as.factor(df_ps$duet_outcome)
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df_ps$foldx_outcome = as.factor(df_ps$foldx_outcome)
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df_ps$ligand_outcome = as.factor(df_ps$ligand_outcome)
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# check
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table(df_ps$mutation_info)
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# further checks to make sure dr and other muts are indeed unique
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dr_muts = df_ps[df_ps$mutation_info == dr_muts_col,]
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dr_muts_names = unique(dr_muts$mutation)
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other_muts = df_ps[df_ps$mutation_info == other_muts_col,]
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other_muts_names = unique(other_muts$mutation)
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if ( table(dr_muts_names%in%other_muts_names)[[1]] == length(dr_muts_names) &&
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table(other_muts_names%in%dr_muts_names)[[1]] == length(other_muts_names) ){
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cat("PASS: dr and other muts are indeed unique")
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}else{
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cat("FAIL: dr adn others muts are NOT unique!")
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quit()
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}
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#%%%%%%%%%%%%%%%%%%%
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# REASSIGNMENT: LIG
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#%%%%%%%%%%%%%%%%%%%%
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df_lig = merged_df3_lig
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# name tidying
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df_lig$mutation_info = as.factor(df_lig$mutation_info)
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df_lig$duet_outcome = as.factor(df_lig$duet_outcome)
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#df_lig$ligand_outcome = as.factor(df_lig$ligand_outcome)
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# check
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table(df_lig$mutation_info)
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#========================================================================
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#===========
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# Data: ps
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#===========
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# keep similar dtypes cols together
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cols_to_select_ps = c("mutationinformation", "mutation", "position", "mutation_info"
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, "duet_outcome"
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, "duet_scaled"
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, "ligand_distance"
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, "asa"
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, "rsa"
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, "rd_values"
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, "kd_values")
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df_wf_ps = df_ps[, cols_to_select_ps]
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pivot_cols_ps = cols_to_select_ps[1:5]; pivot_cols_ps
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expected_rows_lf_ps = nrow(df_wf_ps) * (length(df_wf_ps) - length(pivot_cols_ps))
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expected_rows_lf_ps
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# LF data: duet
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df_lf_ps = gather(df_wf_ps, param_type, param_value, duet_scaled:kd_values, factor_key=TRUE)
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if (nrow(df_lf_ps) == expected_rows_lf_ps){
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cat("PASS: long format data created for duet")
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}else{
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cat("FAIL: long format data could not be created for duet")
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exit()
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}
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str(df_wf_ps)
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str(df_lf_ps)
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# assign pretty labels: param_type
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levels(df_lf_ps$param_type); table(df_lf_ps$param_type)
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ligand_dist_colname = paste0("Distance to ligand (", angstroms_symbol, ")")
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ligand_dist_colname
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duet_stability_name = paste0(delta_symbol, delta_symbol, "G")
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duet_stability_name
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#levels(df_lf_ps$param_type)[levels(df_lf_ps$param_type)=="duet_scaled"] <- "Stability"
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levels(df_lf_ps$param_type)[levels(df_lf_ps$param_type)=="duet_scaled"] <- duet_stability_name
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#levels(df_lf_ps$param_type)[levels(df_lf_ps$param_type)=="ligand_distance"] <- "Ligand Distance"
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levels(df_lf_ps$param_type)[levels(df_lf_ps$param_type)=="ligand_distance"] <- ligand_dist_colname
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levels(df_lf_ps$param_type)[levels(df_lf_ps$param_type)=="asa"] <- "ASA"
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levels(df_lf_ps$param_type)[levels(df_lf_ps$param_type)=="rsa"] <- "RSA"
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levels(df_lf_ps$param_type)[levels(df_lf_ps$param_type)=="rd_values"] <- "RD"
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levels(df_lf_ps$param_type)[levels(df_lf_ps$param_type)=="kd_values"] <- "KD"
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# check
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levels(df_lf_ps$param_type); table(df_lf_ps$param_type)
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# assign pretty labels: mutation_info
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levels(df_lf_ps$mutation_info); table(df_lf_ps$mutation_info)
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sum(table(df_lf_ps$mutation_info)) == nrow(df_lf_ps)
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levels(df_lf_ps$mutation_info)[levels(df_lf_ps$mutation_info)==dr_muts_col] <- "DM"
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levels(df_lf_ps$mutation_info)[levels(df_lf_ps$mutation_info)==other_muts_col] <- "OM"
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# check
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levels(df_lf_ps$mutation_info); table(df_lf_ps$mutation_info)
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############################################################################
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#===========
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# LF data: LIG
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#===========
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# keep similar dtypes cols together
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cols_to_select_lig = c("mutationinformation", "mutation", "position", "mutation_info"
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, "ligand_outcome"
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, "affinity_scaled"
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#, "ligand_distance"
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, "asa"
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, "rsa"
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, "rd_values"
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, "kd_values")
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df_wf_lig = df_lig[, cols_to_select_lig]
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pivot_cols_lig = cols_to_select_lig[1:5]; pivot_cols_lig
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expected_rows_lf_lig = nrow(df_wf_lig) * (length(df_wf_lig) - length(pivot_cols_lig))
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expected_rows_lf_lig
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# LF data: foldx
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df_lf_lig = gather(df_wf_lig, param_type, param_value, affinity_scaled:kd_values, factor_key=TRUE)
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if (nrow(df_lf_lig) == expected_rows_lf_lig){
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cat("PASS: long format data created for foldx")
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}else{
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cat("FAIL: long format data could not be created for foldx")
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exit()
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}
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# assign pretty labels: param_type
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levels(df_lf_lig$param_type); table(df_lf_lig$param_type)
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levels(df_lf_lig$param_type)[levels(df_lf_lig$param_type)=="affinity_scaled"] <- "Ligand Affinity"
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#levels(df_lf_lig$param_type)[levels(df_lf_lig$param_type)=="ligand_distance"] <- "Ligand Distance"
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levels(df_lf_lig$param_type)[levels(df_lf_lig$param_type)=="asa"] <- "ASA"
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levels(df_lf_lig$param_type)[levels(df_lf_lig$param_type)=="rsa"] <- "RSA"
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levels(df_lf_lig$param_type)[levels(df_lf_lig$param_type)=="rd_values"] <- "RD"
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levels(df_lf_lig$param_type)[levels(df_lf_lig$param_type)=="kd_values"] <- "KD"
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#check
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levels(df_lf_lig$param_type); table(df_lf_lig$param_type)
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# assign pretty labels: mutation_info
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levels(df_lf_lig$mutation_info); table(df_lf_lig$mutation_info)
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sum(table(df_lf_lig$mutation_info)) == nrow(df_lf_lig)
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levels(df_lf_lig$mutation_info)[levels(df_lf_lig$mutation_info)==dr_muts_col] <- "DM"
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levels(df_lf_lig$mutation_info)[levels(df_lf_lig$mutation_info)==other_muts_col] <- "OM"
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# check
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levels(df_lf_lig$mutation_info); table(df_lf_lig$mutation_info)
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#############################################################################
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#===========
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# Data: foldx
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#===========
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# keep similar dtypes cols together
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cols_to_select_foldx = c("mutationinformation", "mutation", "position", "mutation_info"
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, "foldx_outcome"
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, "foldx_scaled")
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#, "ligand_distance"
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#, "asa"
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#, "rsa"
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#, "rd_values"
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#, "kd_values")
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df_wf_foldx = df_ps[, cols_to_select_foldx]
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pivot_cols_foldx = cols_to_select_foldx[1:5]; pivot_cols_foldx
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expected_rows_lf_foldx = nrow(df_wf_foldx) * (length(df_wf_foldx) - length(pivot_cols_foldx))
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expected_rows_lf_foldx
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# LF data: foldx
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df_lf_foldx = gather(df_wf_foldx, param_type, param_value, foldx_scaled, factor_key=TRUE)
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if (nrow(df_lf_foldx) == expected_rows_lf_foldx){
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cat("PASS: long format data created for foldx")
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}else{
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cat("FAIL: long format data could not be created for foldx")
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exit()
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}
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foldx_stability_name = paste0(delta_symbol, delta_symbol, "G")
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foldx_stability_name
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# assign pretty labels: param type
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levels(df_lf_foldx$param_type); table(df_lf_foldx$param_type)
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#levels(df_lf_foldx$param_type)[levels(df_lf_foldx$param_type)=="foldx_scaled"] <- "Stability"
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levels(df_lf_foldx$param_type)[levels(df_lf_foldx$param_type)=="foldx_scaled"] <- foldx_stability_name
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#levels(df_lf_foldx$param_type)[levels(df_lf_foldx$param_type)=="ligand_distance"] <- "Ligand Distance"
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#levels(df_lf_foldx$param_type)[levels(df_lf_foldx$param_type)=="asa"] <- "ASA"
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#levels(df_lf_foldx$param_type)[levels(df_lf_foldx$param_type)=="rsa"] <- "RSA"
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#levels(df_lf_foldx$param_type)[levels(df_lf_foldx$param_type)=="rd_values"] <- "RD"
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#levels(df_lf_foldx$param_type)[levels(df_lf_foldx$param_type)=="kd_values"] <- "KD"
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# check
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levels(df_lf_foldx$param_type); table(df_lf_foldx$param_type)
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# assign pretty labels: mutation_info
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levels(df_lf_foldx$mutation_info); table(df_lf_foldx$mutation_info)
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sum(table(df_lf_foldx$mutation_info)) == nrow(df_lf_foldx)
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levels(df_lf_foldx$mutation_info)[levels(df_lf_foldx$mutation_info)==dr_muts_col] <- "DM"
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levels(df_lf_foldx$mutation_info)[levels(df_lf_foldx$mutation_info)==other_muts_col] <- "OM"
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# check
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levels(df_lf_foldx$mutation_info); table(df_lf_foldx$mutation_info)
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############################################################################
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# clear excess variables
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rm(cols_to_select_ps, cols_to_select_foldx, cols_to_select_lig
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, pivot_cols_ps, pivot_cols_foldx, pivot_cols_lig
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, expected_rows_lf_ps, expected_rows_lf_foldx, expected_rows_lf_lig
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, my_max, my_min, na_count, na_count_df2, na_count_df3, dup_muts_nu
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, c1, c2, n)
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