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annotate 0.7.0/bin/gen_salmon_res_table.py @ 21:4ce0e079377d tip

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planemo upload
author kkonganti
date Mon, 15 Jul 2024 12:01:00 -0400
parents 0e7a0053e4a6
children
rev   line source
kkonganti@17 1 #!/usr/bin/env python3
kkonganti@17 2
kkonganti@17 3 # Kranti Konganti
kkonganti@17 4
kkonganti@17 5 import argparse
kkonganti@17 6 import glob
kkonganti@17 7 import inspect
kkonganti@17 8 import json
kkonganti@17 9 import logging
kkonganti@17 10 import os
kkonganti@17 11 import pickle
kkonganti@17 12 import pprint
kkonganti@17 13 import re
kkonganti@17 14 from collections import defaultdict
kkonganti@17 15
kkonganti@17 16 import yaml
kkonganti@17 17
kkonganti@17 18
kkonganti@17 19 # Multiple inheritence for pretty printing of help text.
kkonganti@17 20 class MultiArgFormatClasses(argparse.RawTextHelpFormatter, argparse.ArgumentDefaultsHelpFormatter):
kkonganti@17 21 pass
kkonganti@17 22
kkonganti@17 23
kkonganti@17 24 # Main
kkonganti@17 25 def main() -> None:
kkonganti@17 26 """
kkonganti@17 27 The succesful execution of this script requires access to bettercallsal formatted
kkonganti@17 28 db flat files. On raven2, they are at /hpc/db/bettercallsall/PDGXXXXXXXXXX.XXXXX
kkonganti@17 29
kkonganti@17 30 It takes the ACC2SERO.pickle file and *.reference_target.cluster_list.tsv file
kkonganti@17 31 for that particular NCBI Pathogens release from the db directory mentioned with
kkonganti@17 32 -db option and a root parent directory of the `salmon quant` results mentioned
kkonganti@17 33 with -sal option and generates a final results table with number of reads
kkonganti@17 34 mapped and a .json file to be used with MultiQC to generate a stacked bar plot.
kkonganti@17 35
kkonganti@17 36 Using -url option optionally adds an extra column of NCBI Pathogens Isolates
kkonganti@17 37 Browser, which directly links out to NCBI Pathogens Isolates SNP viewer tool.
kkonganti@17 38 """
kkonganti@17 39 # Set logging.
kkonganti@17 40 logging.basicConfig(
kkonganti@17 41 format="\n" + "=" * 55 + "\n%(asctime)s - %(levelname)s\n" + "=" * 55 + "\n%(message)s\n\n",
kkonganti@17 42 level=logging.DEBUG,
kkonganti@17 43 )
kkonganti@17 44
kkonganti@17 45 # Debug print.
kkonganti@17 46 ppp = pprint.PrettyPrinter(width=55)
kkonganti@17 47 prog_name = inspect.stack()[0].filename
kkonganti@17 48
kkonganti@17 49 parser = argparse.ArgumentParser(
kkonganti@17 50 prog=prog_name, description=main.__doc__, formatter_class=MultiArgFormatClasses
kkonganti@17 51 )
kkonganti@17 52
kkonganti@17 53 required = parser.add_argument_group("required arguments")
kkonganti@17 54
kkonganti@17 55 required.add_argument(
kkonganti@17 56 "-sal",
kkonganti@17 57 dest="salmon_res_dir",
kkonganti@17 58 default=False,
kkonganti@17 59 required=True,
kkonganti@17 60 help="Absolute UNIX path to the parent directory that contains the\n"
kkonganti@17 61 + "`salmon quant` results directory. For example, if path to\n"
kkonganti@17 62 + "`quant.sf` is in /hpc/john_doe/test/salmon_res/quant.sf, then\n"
kkonganti@17 63 + "use this command-line option as:\n"
kkonganti@17 64 + "-sal /hpc/john_doe/test",
kkonganti@17 65 )
kkonganti@17 66 required.add_argument(
kkonganti@17 67 "-snp",
kkonganti@17 68 dest="rtc",
kkonganti@17 69 default=False,
kkonganti@17 70 required=True,
kkonganti@17 71 help="Absolute UNIX Path to the PDG SNP reference target cluster\n"
kkonganti@17 72 + "metadata file. On raven2, these are located at\n"
kkonganti@17 73 + "/hpc/db/bettercallsal/PDGXXXXXXXXXX.XXXXX\n"
kkonganti@17 74 + "Required if -sal is on.",
kkonganti@17 75 )
kkonganti@17 76 required.add_argument(
kkonganti@17 77 "-pickle",
kkonganti@17 78 dest="acc2sero",
kkonganti@17 79 default=False,
kkonganti@17 80 required=True,
kkonganti@17 81 help="Absolute UNIX Path to the *ACC2SERO.pickle\n"
kkonganti@17 82 + "metadata file. On raven2, these are located at\n"
kkonganti@17 83 + "/hpc/db/bettercallsal/PDGXXXXXXXXXX.XXXXX\n"
kkonganti@17 84 + "Required if -sal is on.",
kkonganti@17 85 )
kkonganti@17 86 parser.add_argument(
kkonganti@17 87 "-op",
kkonganti@17 88 dest="out_prefix",
kkonganti@17 89 default="bettercallsal.tblsum",
kkonganti@17 90 required=False,
kkonganti@17 91 help="Set the output file(s) prefix for output(s) generated\n" + "by this program.",
kkonganti@17 92 )
kkonganti@17 93 parser.add_argument(
kkonganti@17 94 "-url",
kkonganti@17 95 dest="show_snp_clust_info",
kkonganti@17 96 default=False,
kkonganti@17 97 required=False,
kkonganti@17 98 action="store_true",
kkonganti@17 99 help="Show SNP cluster participation information of the final genome hit.\n"
kkonganti@17 100 + "This may be useful to see a relative placement of your sample in\n"
kkonganti@17 101 + "NCBI Isolates SNP Tree Viewer based on genome similarity but however\n"
kkonganti@17 102 + "due to rapid nature of the updates at NCBI Pathogen Detection Project,\n"
kkonganti@17 103 + "the placement may be in an outdated cluster.",
kkonganti@17 104 )
kkonganti@17 105
kkonganti@17 106 args = parser.parse_args()
kkonganti@17 107 salmon_res_dir = args.salmon_res_dir
kkonganti@17 108 out_prefix = args.out_prefix
kkonganti@17 109 show_snp_clust_col = args.show_snp_clust_info
kkonganti@17 110 rtc = args.rtc
kkonganti@17 111 pickled_sero = args.acc2sero
kkonganti@17 112 no_hit = "No genome hit"
kkonganti@17 113 no_presence = "Salmonella presence not detected"
kkonganti@17 114 bcs_sal_yn_prefix = "bettercallsal_salyn"
kkonganti@17 115 sal_y = "Detected"
kkonganti@17 116 sal_n = "Not detected"
kkonganti@17 117 null_value = "NULL"
kkonganti@17 118 assm_pat = re.compile(r"GC[AF]\_[0-9]+\.*[0-9]*")
kkonganti@17 119 ncbi_pathogens_base_url = "https://www.ncbi.nlm.nih.gov/pathogens/"
kkonganti@17 120 ncbi_pathogens_genome_base = "https://www.ncbi.nlm.nih.gov/datasets/genome/"
kkonganti@17 121
kkonganti@17 122 sample2salmon, snp_clusters, multiqc_salmon_counts, seen_sero, sal_yn = (
kkonganti@17 123 defaultdict(defaultdict),
kkonganti@17 124 defaultdict(defaultdict),
kkonganti@17 125 defaultdict(defaultdict),
kkonganti@17 126 defaultdict(int),
kkonganti@17 127 defaultdict(int),
kkonganti@17 128 )
kkonganti@17 129
kkonganti@17 130 cell_colors_yml = {
kkonganti@17 131 bcs_sal_yn_prefix: {sal_y: "#c8e6c9 !important;", sal_n: "#ffcdd2 !important;"}
kkonganti@17 132 }
kkonganti@17 133
kkonganti@17 134 salmon_comb_res = os.path.join(os.getcwd(), out_prefix + ".txt")
kkonganti@17 135 bcs_sal_yn = re.sub(out_prefix, bcs_sal_yn_prefix + ".tblsum", salmon_comb_res)
kkonganti@17 136 cell_colors_yml_file = re.sub(
kkonganti@17 137 out_prefix + ".txt", bcs_sal_yn_prefix + ".cellcolors.yml", salmon_comb_res
kkonganti@17 138 )
kkonganti@17 139 salmon_comb_res_mqc = os.path.join(os.getcwd(), str(out_prefix).split(".")[0] + "_mqc.json")
kkonganti@17 140 salmon_res_files = glob.glob(os.path.join(salmon_res_dir, "*", "quant.sf"), recursive=True)
kkonganti@17 141 salmon_res_file_failed = glob.glob(os.path.join(salmon_res_dir, "BCS_NO_CALLS.txt"))
kkonganti@17 142
kkonganti@17 143 if rtc and (not os.path.exists(rtc) or not os.path.getsize(rtc) > 0):
kkonganti@17 144 logging.error(
kkonganti@17 145 "The reference target cluster metadata file,\n"
kkonganti@17 146 + f"{os.path.basename(rtc)} does not exist or is empty!"
kkonganti@17 147 )
kkonganti@17 148 exit(1)
kkonganti@17 149
kkonganti@17 150 if rtc and (not salmon_res_dir or not pickled_sero):
kkonganti@17 151 logging.error("When -rtc is on, -sal and -ps are also required.")
kkonganti@17 152 exit(1)
kkonganti@17 153
kkonganti@17 154 if pickled_sero and (not os.path.exists(pickled_sero) or not os.path.getsize(pickled_sero)):
kkonganti@17 155 logging.error(
kkonganti@17 156 "The pickle file,\n" + f"{os.path.basename(pickled_sero)} does not exist or is empty!"
kkonganti@17 157 )
kkonganti@17 158 exit(1)
kkonganti@17 159
kkonganti@17 160 if salmon_res_dir:
kkonganti@17 161 if not os.path.isdir(salmon_res_dir):
kkonganti@17 162 logging.error("UNIX path\n" + f"{salmon_res_dir}\n" + "does not exist!")
kkonganti@17 163 exit(1)
kkonganti@17 164 if len(salmon_res_files) <= 0:
kkonganti@17 165 # logging.error(
kkonganti@17 166 # "Parent directory,\n"
kkonganti@17 167 # + f"{salmon_res_dir}"
kkonganti@17 168 # + "\ndoes not seem to have any directories that contain\n"
kkonganti@17 169 # + "the `quant.sf` file(s)."
kkonganti@17 170 # )
kkonganti@17 171 # exit(1)
kkonganti@17 172 with open(salmon_comb_res, "w") as salmon_comb_res_fh:
kkonganti@17 173 salmon_comb_res_fh.write(f"Sample\n{no_hit}s in any samples\n")
kkonganti@17 174 salmon_comb_res_fh.close()
kkonganti@17 175
kkonganti@17 176 with open(bcs_sal_yn, "w") as bcs_sal_yn_fh:
kkonganti@17 177 bcs_sal_yn_fh.write(f"Sample\n{no_presence} in any samples\n")
kkonganti@17 178 bcs_sal_yn_fh.close()
kkonganti@17 179
kkonganti@17 180 exit(0)
kkonganti@17 181
kkonganti@17 182 if rtc and os.path.exists(rtc) and os.path.getsize(rtc) > 0:
kkonganti@17 183
kkonganti@17 184 # pdg_release = re.match(r"(^PDG\d+\.\d+)\..+", os.path.basename(rtc))[1] + "/"
kkonganti@17 185 acc2sero = pickle.load(file=open(pickled_sero, "rb"))
kkonganti@17 186
kkonganti@17 187 with open(rtc, "r") as rtc_fh:
kkonganti@17 188
kkonganti@17 189 for line in rtc_fh:
kkonganti@17 190 cols = line.strip().split("\t")
kkonganti@17 191
kkonganti@17 192 if len(cols) < 4:
kkonganti@17 193 logging.error(
kkonganti@17 194 f"The file {os.path.basename(rtc)} seems to\n"
kkonganti@17 195 + "be malformed. It contains less than required 4 columns."
kkonganti@17 196 )
kkonganti@17 197 exit(1)
kkonganti@17 198 elif cols[3] != null_value:
kkonganti@17 199 snp_clusters[cols[0]].setdefault("assembly_accs", []).append(cols[3])
kkonganti@17 200 snp_clusters[cols[3]].setdefault("snp_clust_id", []).append(cols[0])
kkonganti@17 201 snp_clusters[cols[3]].setdefault("pathdb_acc_id", []).append(cols[1])
kkonganti@17 202 if len(snp_clusters[cols[3]]["snp_clust_id"]) > 1:
kkonganti@17 203 logging.error(
kkonganti@17 204 f"There is a duplicate reference accession [{cols[3]}]"
kkonganti@17 205 + f"in the metadata file{os.path.basename(rtc)}!"
kkonganti@17 206 )
kkonganti@17 207 exit(1)
kkonganti@17 208
kkonganti@17 209 rtc_fh.close()
kkonganti@17 210
kkonganti@17 211 for salmon_res_file in salmon_res_files:
kkonganti@17 212 sample_name = re.match(
kkonganti@17 213 r"(^.+?)((\_salmon\_res)|(\.salmon))$",
kkonganti@17 214 os.path.basename(os.path.dirname(salmon_res_file)),
kkonganti@17 215 )[1]
kkonganti@17 216 salmon_meta_json = os.path.join(
kkonganti@17 217 os.path.dirname(salmon_res_file), "aux_info", "meta_info.json"
kkonganti@17 218 )
kkonganti@17 219
kkonganti@17 220 if not os.path.exists(salmon_meta_json) or not os.path.getsize(salmon_meta_json) > 0:
kkonganti@17 221 logging.error(
kkonganti@17 222 "The file\n"
kkonganti@17 223 + f"{salmon_meta_json}\ndoes not exist or is empty!\n"
kkonganti@17 224 + "Did `salmon quant` fail?"
kkonganti@17 225 )
kkonganti@17 226 exit(1)
kkonganti@17 227
kkonganti@17 228 if not os.path.exists(salmon_res_file) or not os.path.getsize(salmon_res_file):
kkonganti@17 229 logging.error(
kkonganti@17 230 "The file\n"
kkonganti@17 231 + f"{salmon_res_file}\ndoes not exist or is empty!\n"
kkonganti@17 232 + "Did `salmon quant` fail?"
kkonganti@17 233 )
kkonganti@17 234 exit(1)
kkonganti@17 235
kkonganti@17 236 with open(salmon_res_file, "r") as salmon_res_fh:
kkonganti@17 237 for line in salmon_res_fh.readlines():
kkonganti@17 238 if re.match(r"^Name.+", line):
kkonganti@17 239 continue
kkonganti@17 240 cols = line.strip().split("\t")
kkonganti@17 241 ref_acc = "_".join(cols[0].split("_")[:2])
kkonganti@17 242
kkonganti@17 243 if ref_acc not in snp_clusters.keys():
kkonganti@17 244 snp_clusters[ref_acc]["snp_clust_id"] = ref_acc
kkonganti@17 245 snp_clusters[ref_acc]["pathdb_acc_id"] = ref_acc
kkonganti@17 246
kkonganti@17 247 (
kkonganti@17 248 sample2salmon[sample_name]
kkonganti@17 249 .setdefault(acc2sero[cols[0]], [])
kkonganti@17 250 .append(int(round(float(cols[4]), 2)))
kkonganti@17 251 )
kkonganti@17 252 (
kkonganti@17 253 sample2salmon[sample_name]
kkonganti@17 254 .setdefault("snp_clust_ids", {})
kkonganti@17 255 .setdefault("".join(snp_clusters[ref_acc]["snp_clust_id"]), [])
kkonganti@17 256 .append("".join(snp_clusters[ref_acc]["pathdb_acc_id"]))
kkonganti@17 257 )
kkonganti@17 258 seen_sero[acc2sero[cols[0]]] = 1
kkonganti@17 259
kkonganti@17 260 salmon_meta_json_read = json.load(open(salmon_meta_json, "r"))
kkonganti@17 261 (
kkonganti@17 262 sample2salmon[sample_name]
kkonganti@17 263 .setdefault("tot_reads", [])
kkonganti@17 264 .append(salmon_meta_json_read["num_processed"])
kkonganti@17 265 )
kkonganti@17 266
kkonganti@17 267 with open(salmon_comb_res, "w") as salmon_comb_res_fh:
kkonganti@17 268
kkonganti@17 269 # snp_clust_col_header = (
kkonganti@17 270 # "\tSNP Cluster(s) by Genome Hit\n" if show_snp_clust_col else "\n"
kkonganti@17 271 # )
kkonganti@17 272 snp_clust_col_header = (
kkonganti@17 273 "\tNCBI Pathogens Isolate Browser\n" if show_snp_clust_col else "\n"
kkonganti@17 274 )
kkonganti@17 275 serotypes = sorted(seen_sero.keys())
kkonganti@17 276 formatted_serotypes = [
kkonganti@17 277 re.sub(r"\,antigen_formula=", " | ", s)
kkonganti@17 278 for s in [re.sub(r"serotype=", "", s) for s in serotypes]
kkonganti@17 279 ]
kkonganti@17 280 salmon_comb_res_fh.write(
kkonganti@17 281 "Sample\t" + "\t".join(formatted_serotypes) + snp_clust_col_header
kkonganti@17 282 )
kkonganti@17 283 # sample_snp_relation = (
kkonganti@17 284 # ncbi_pathogens_base_url
kkonganti@17 285 # + pdg_release
kkonganti@17 286 # + "".join(snp_clusters[ref_acc]["snp_clust_id"])
kkonganti@17 287 # + "?accessions="
kkonganti@17 288 # )
kkonganti@17 289 if len(salmon_res_file_failed) == 1:
kkonganti@17 290 with (open("".join(salmon_res_file_failed), "r")) as no_calls_fh:
kkonganti@17 291 for line in no_calls_fh.readlines():
kkonganti@17 292 if line in ["\n", "\n\r", "\r"]:
kkonganti@17 293 continue
kkonganti@17 294 salmon_comb_res_fh.write(line.strip())
kkonganti@17 295 sal_yn[line.strip()] += 0
kkonganti@17 296 for serotype in serotypes:
kkonganti@17 297 salmon_comb_res_fh.write("\t-")
kkonganti@17 298 salmon_comb_res_fh.write(
kkonganti@17 299 "\t-\n"
kkonganti@17 300 ) if show_snp_clust_col else salmon_comb_res_fh.write("\n")
kkonganti@17 301 no_calls_fh.close()
kkonganti@17 302
kkonganti@17 303 for sample, counts in sorted(sample2salmon.items()):
kkonganti@17 304 salmon_comb_res_fh.write(sample)
kkonganti@17 305 snp_cluster_res_col = list()
kkonganti@17 306
kkonganti@17 307 for snp_clust_id in sample2salmon[sample]["snp_clust_ids"].keys():
kkonganti@17 308 # print(snp_clust_id)
kkonganti@17 309 # print(",".join(sample2salmon[sample]["snp_clust_ids"][snp_clust_id]))
kkonganti@17 310 # ppp.pprint(sample2salmon[sample]["snp_clust_ids"])
kkonganti@17 311 # ppp.pprint(sample2salmon[sample]["snp_clust_ids"][snp_clust_id])
kkonganti@17 312 # final_url_text = ",".join(
kkonganti@17 313 # sample2salmon[sample]["snp_clust_ids"][snp_clust_id]
kkonganti@17 314 # )
kkonganti@17 315 # final_url_text_to_show = snp_clust_id
kkonganti@17 316 # snp_cluster_res_col.append(
kkonganti@17 317 # "".join(
kkonganti@17 318 # [
kkonganti@17 319 # f'<a href="',
kkonganti@17 320 # sample_snp_relation,
kkonganti@17 321 # ",".join(sample2salmon[sample]["snp_clust_ids"][snp_clust_id]),
kkonganti@17 322 # f'" target="_blank">{snp_clust_id}</a>',
kkonganti@17 323 # ]
kkonganti@17 324 # )
kkonganti@17 325 # )
kkonganti@17 326 # ppp.pprint(sample2salmon[sample])
kkonganti@17 327 for pathdbacc in sample2salmon[sample]["snp_clust_ids"][snp_clust_id]:
kkonganti@17 328 # final_url_text_to_show = " ".join(
kkonganti@17 329 # sample2salmon[sample]["snp_clust_ids"][snp_clust_id]
kkonganti@17 330 # )
kkonganti@17 331 sample_snp_relation = (
kkonganti@17 332 ncbi_pathogens_genome_base
kkonganti@17 333 if assm_pat.match(pathdbacc)
kkonganti@17 334 else ncbi_pathogens_base_url + "isolates/#"
kkonganti@17 335 )
kkonganti@17 336
kkonganti@17 337 snp_cluster_res_col.append(
kkonganti@17 338 "".join(
kkonganti@17 339 [
kkonganti@17 340 f'<a href="',
kkonganti@17 341 sample_snp_relation,
kkonganti@17 342 pathdbacc,
kkonganti@17 343 f'" target="_blank">{pathdbacc}</a>',
kkonganti@17 344 ]
kkonganti@17 345 )
kkonganti@17 346 )
kkonganti@17 347
kkonganti@17 348 per_serotype_counts = 0
kkonganti@17 349 for serotype in serotypes:
kkonganti@17 350
kkonganti@17 351 if serotype in sample2salmon[sample].keys():
kkonganti@17 352 # ppp.pprint(counts)
kkonganti@17 353 sample_perc_mapped = round(
kkonganti@17 354 sum(counts[serotype]) / sum(counts["tot_reads"]) * 100, 2
kkonganti@17 355 )
kkonganti@17 356 salmon_comb_res_fh.write(
kkonganti@17 357 f"\t{sum(counts[serotype])} ({sample_perc_mapped}%)"
kkonganti@17 358 )
kkonganti@17 359 multiqc_salmon_counts[sample].setdefault(
kkonganti@17 360 re.match(r"^serotype=(.+?)\,antigen_formula.*", serotype)[1],
kkonganti@17 361 sum(counts[serotype]),
kkonganti@17 362 )
kkonganti@17 363 per_serotype_counts += sum(counts[serotype])
kkonganti@17 364 sal_yn[sample] += 1
kkonganti@17 365 else:
kkonganti@17 366 salmon_comb_res_fh.write(f"\t-")
kkonganti@17 367 sal_yn[sample] += 0
kkonganti@17 368
kkonganti@17 369 multiqc_salmon_counts[sample].setdefault(
kkonganti@17 370 no_hit, sum(counts["tot_reads"]) - per_serotype_counts
kkonganti@17 371 )
kkonganti@17 372 snp_clust_col_val = (
kkonganti@17 373 f'\t{" ".join(snp_cluster_res_col)}\n' if show_snp_clust_col else "\n"
kkonganti@17 374 )
kkonganti@17 375 # ppp.pprint(multiqc_salmon_counts)
kkonganti@17 376 salmon_comb_res_fh.write(snp_clust_col_val)
kkonganti@17 377
kkonganti@17 378 with open(bcs_sal_yn, "w") as bcs_sal_yn_fh:
kkonganti@17 379 bcs_sal_yn_fh.write("Sample\tSalmonella Presence\tNo. of Serotypes\n")
kkonganti@17 380 for sample in sal_yn.keys():
kkonganti@17 381 if sal_yn[sample] > 0:
kkonganti@17 382 bcs_sal_yn_fh.write(f"{sample}\tDetected\t{sal_yn[sample]}\n")
kkonganti@17 383 else:
kkonganti@17 384 bcs_sal_yn_fh.write(f"{sample}\tNot detected\t{sal_yn[sample]}\n")
kkonganti@17 385
kkonganti@17 386 with open(cell_colors_yml_file, "w") as cell_colors_fh:
kkonganti@17 387 yaml.dump(cell_colors_yml, cell_colors_fh, default_flow_style=False)
kkonganti@17 388
kkonganti@17 389 salmon_plot_json(salmon_comb_res_mqc, multiqc_salmon_counts, no_hit)
kkonganti@17 390
kkonganti@17 391 salmon_comb_res_fh.close()
kkonganti@17 392 bcs_sal_yn_fh.close()
kkonganti@17 393 cell_colors_fh.close()
kkonganti@17 394
kkonganti@17 395
kkonganti@17 396 def salmon_plot_json(file: None, sample_salmon_counts: None, no_hit: None) -> None:
kkonganti@17 397 """
kkonganti@17 398 This method will take a dictionary of salmon counts per sample
kkonganti@17 399 and will dump a JSON that will be used by MultiQC.
kkonganti@17 400 """
kkonganti@17 401
kkonganti@17 402 if file is None or sample_salmon_counts is None:
kkonganti@17 403 logging.error(
kkonganti@17 404 "Neither an output file to dump the JSON for MultiQC or the"
kkonganti@17 405 + "dictionary holding the salmon counts was not passed."
kkonganti@17 406 )
kkonganti@17 407
kkonganti@17 408 # Credit: http://phrogz.net/tmp/24colors.html
kkonganti@17 409 # Will cycle through 20 distinct colors.
kkonganti@17 410 distinct_color_palette = [
kkonganti@17 411 "#FF0000",
kkonganti@17 412 "#FFFF00",
kkonganti@17 413 "#00EAFF",
kkonganti@17 414 "#AA00FF",
kkonganti@17 415 "#FF7F00",
kkonganti@17 416 "#BFFF00",
kkonganti@17 417 "#0095FF",
kkonganti@17 418 "#FF00AA",
kkonganti@17 419 "#FFD400",
kkonganti@17 420 "#6AFF00",
kkonganti@17 421 "#0040FF",
kkonganti@17 422 "#EDB9B9",
kkonganti@17 423 "#B9D7ED",
kkonganti@17 424 "#E7E9B9",
kkonganti@17 425 "#DCB9ED",
kkonganti@17 426 "#B9EDE0",
kkonganti@17 427 "#8F2323",
kkonganti@17 428 "#23628F",
kkonganti@17 429 "#8F6A23",
kkonganti@17 430 "#6B238F",
kkonganti@17 431 "#4F8F23",
kkonganti@17 432 ]
kkonganti@17 433
kkonganti@17 434 # Credit: https://mokole.com/palette.html
kkonganti@17 435 # Will use this palette if we run out ouf
kkonganti@17 436 # 20 serotypes. More than 50 serotypes
kkonganti@17 437 # per run is probably rare but if not,
kkonganti@17 438 # will cycle through about 45.
kkonganti@17 439 distinct_color_palette2 = [
kkonganti@17 440 "#2F4F4F", # darkslategray
kkonganti@17 441 "#556B2F", # darkolivegreen
kkonganti@17 442 "#A0522D", # sienna
kkonganti@17 443 "#2E8B57", # seagreen
kkonganti@17 444 "#006400", # darkgreen
kkonganti@17 445 "#8B0000", # darkred
kkonganti@17 446 "#808000", # olive
kkonganti@17 447 "#BC8F8F", # rosybrown
kkonganti@17 448 "#663399", # rebeccapurple
kkonganti@17 449 "#B8860B", # darkgoldenrod
kkonganti@17 450 "#4682B4", # steelblue
kkonganti@17 451 "#000080", # navy
kkonganti@17 452 "#D2691E", # chocolate
kkonganti@17 453 "#9ACD32", # yellowgreen
kkonganti@17 454 "#20B2AA", # lightseagreen
kkonganti@17 455 "#CD5C5C", # indianred
kkonganti@17 456 "#8FBC8F", # darkseagreen
kkonganti@17 457 "#800080", # purple
kkonganti@17 458 "#B03060", # maroon3
kkonganti@17 459 "#FF8C00", # darkorange
kkonganti@17 460 "#FFD700", # gold
kkonganti@17 461 "#FFFF00", # yellow
kkonganti@17 462 "#DEB887", # burlywood
kkonganti@17 463 "#00FF00", # lime
kkonganti@17 464 "#BA55D3", # mediumorchid
kkonganti@17 465 "#00FA9A", # mediumspringgreen
kkonganti@17 466 "#4169E1", # royalblue
kkonganti@17 467 "#E9967A", # darksalmon
kkonganti@17 468 "#DC143C", # crimson
kkonganti@17 469 "#00FFFF", # aqua
kkonganti@17 470 "#F4A460", # sandybrown
kkonganti@17 471 "#9370DB", # mediumpurple
kkonganti@17 472 "#0000FF", # blue
kkonganti@17 473 "#ADFF2F", # greenyellow
kkonganti@17 474 "#FF6347", # tomato
kkonganti@17 475 "#D8BFD8", # thistle
kkonganti@17 476 "#FF00FF", # fuchsia
kkonganti@17 477 "#DB7093", # palevioletred
kkonganti@17 478 "#F0E68C", # khaki
kkonganti@17 479 "#6495ED", # cornflower
kkonganti@17 480 "#DDA0DD", # plum
kkonganti@17 481 "#EE82EE", # violet
kkonganti@17 482 "#7FFFD4", # aquamarine
kkonganti@17 483 "#FAFAD2", # lightgoldenrod
kkonganti@17 484 "#FF69B4", # hotpink
kkonganti@17 485 "#FFB6C1", # lightpink
kkonganti@17 486 ]
kkonganti@17 487
kkonganti@17 488 no_hit_color = "#434348"
kkonganti@17 489 col_count = 0
kkonganti@17 490 serotypes = set()
kkonganti@17 491 salmon_counts = defaultdict(defaultdict)
kkonganti@17 492 salmon_counts["id"] = "BETTERCALLSAL_SALMON_COUNTS"
kkonganti@17 493 salmon_counts["section_name"] = "Salmon read counts"
kkonganti@17 494 salmon_counts["description"] = (
kkonganti@17 495 "This section shows the read counts from running <code>salmon</code> "
kkonganti@17 496 + "in <code>--meta</code> mode using SE, merged PE or concatenated PE reads against "
kkonganti@17 497 + "an on-the-fly <code>salmon</code> index generated from the genome hits "
kkonganti@17 498 + "of <code>kma</code>."
kkonganti@17 499 )
kkonganti@17 500 salmon_counts["plot_type"] = "bargraph"
kkonganti@17 501 salmon_counts["pconfig"]["id"] = "bettercallsal_salmon_counts_plot"
kkonganti@17 502 salmon_counts["pconfig"]["title"] = "Salmon: Read counts"
kkonganti@17 503 salmon_counts["pconfig"]["ylab"] = "Number of reads"
kkonganti@17 504 salmon_counts["pconfig"]["xDecimals"] = "false"
kkonganti@17 505 salmon_counts["pconfig"]["cpswitch_counts_label"] = "Number of reads (Counts)"
kkonganti@17 506 salmon_counts["pconfig"]["cpswitch_percent_label"] = "Number of reads (Percentages)"
kkonganti@17 507
kkonganti@17 508 for sample in sorted(sample_salmon_counts.keys()):
kkonganti@17 509 serotypes.update(list(sample_salmon_counts[sample].keys()))
kkonganti@17 510 salmon_counts["data"][sample] = sample_salmon_counts[sample]
kkonganti@17 511
kkonganti@17 512 if len(serotypes) > len(distinct_color_palette):
kkonganti@17 513 distinct_color_palette = distinct_color_palette2
kkonganti@17 514
kkonganti@17 515 for serotype in sorted(serotypes):
kkonganti@17 516 if serotype == no_hit:
kkonganti@17 517 continue
kkonganti@17 518 if col_count == len(distinct_color_palette) - 1:
kkonganti@17 519 col_count = 0
kkonganti@17 520
kkonganti@17 521 col_count += 1
kkonganti@17 522 salmon_counts["categories"][serotype] = {"color": distinct_color_palette[col_count]}
kkonganti@17 523
kkonganti@17 524 salmon_counts["categories"][no_hit] = {"color": no_hit_color}
kkonganti@17 525 json.dump(salmon_counts, open(file, "w"))
kkonganti@17 526
kkonganti@17 527
kkonganti@17 528 if __name__ == "__main__":
kkonganti@17 529 main()