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Takes output file generated by VarScan2 somatic programme and converts the formats. See here for updated versions https://github.com/PoisonAlien/varscan_accessories
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__author__ = "Anand M" | |
''' | |
Takes output file generated by VarScan2 somatic programme and converts the formats. | |
''' | |
import argparse, math, re | |
parser = argparse.ArgumentParser( | |
description="Converts VarScan2 somatic vcf to native format and vice-versa.\nInput is automatically detected") | |
parser.add_argument('input', help='Input file generated by VarScan2 somatic') | |
# parser.add_argument('output', help='output file name') | |
args = parser.parse_args() | |
# Function to print header line | |
def printNativeHeader(): | |
""" | |
:rtype : Null | |
""" | |
print( | |
"chrom\tposition\tref\tvar\tnormal_reads1\tnormal_reads2\tnormal_var_freq\tnormal_gt\ttumor_reads1\ttumor_reads\ttumor_var_freq\ttumor_gt\tsomatic_status\tvariant_p_value\tsomatic_p_value\ttumor_reads1_plus\ttumor_reads1_minus\ttumor_reads2_plus\ttumor_reads2_minus\tnormal_reads1_plus\tnormal_reads1_minus\tnormal_reads2_plus\tnormal_reads2_minus") | |
# Function to print vcf header | |
def printVcfHeader(): | |
print("##fileformat=VCFv4.1\n" | |
"##source=VarScan2\n" | |
"##INFO=<ID=DP,Number=1,Type=Integer,Description=\"Total depth of quality bases\">\n" | |
"##INFO=<ID=SOMATIC,Number=0,Type=Flag,Description=\"Indicates if record is a somatic mutation\">\n" | |
"##INFO=<ID=SS,Number=1,Type=String,Description=\"Somatic status of variant (0=Reference,1=Germline,2=Somatic,3=LOH, or 5=Unknown)\">\n" | |
"##INFO=<ID=SSC,Number=1,Type=String,Description=\"Somatic score in Phred scale (0-255) derived from somatic p-value\">\n" | |
"##INFO=<ID=GPV,Number=1,Type=Float,Description=\"Fisher's Exact Test P-value of tumor+normal versus no variant for Germline calls\">\n" | |
"##INFO=<ID=SPV,Number=1,Type=Float,Description=\"Fisher's Exact Test P-value of tumor versus normal for Somatic/LOH calls\">\n" | |
"##FILTER=<ID=str10,Description=\"Less than 10% or more than 90% of variant supporting reads on one strand\">\n" | |
"##FILTER=<ID=indelError,Description=\"Likely artifact due to indel reads at this position\">\n" | |
"##FORMAT=<ID=GT,Number=1,Type=String,Description=\"Genotype\">\n" | |
"##FORMAT=<ID=GQ,Number=1,Type=Integer,Description=\"Genotype Quality\">\n" | |
"##FORMAT=<ID=DP,Number=1,Type=Integer,Description=\"Read Depth\">\n" | |
"##FORMAT=<ID=RD,Number=1,Type=Integer,Description=\"Depth of reference-supporting bases (reads1)\">\n" | |
"##FORMAT=<ID=AD,Number=1,Type=Integer,Description=\"Depth of variant-supporting bases (reads2)\">\n" | |
"##FORMAT=<ID=FREQ,Number=1,Type=String,Description=\"Variant allele frequency\">\n" | |
"##FORMAT=<ID=DP4,Number=1,Type=String,Description=\"Strand read counts: ref/fwd, ref/rev, var/fwd, var/rev\">\n" | |
"#CHROM POS ID REF ALT QUAL FILTER INFO FORMAT NORMAL TUMOR") | |
# Function to convert vcf record to NativeFormat record | |
def makeNativeRec(vcfIp): | |
""" | |
:rtype : Null | |
:type nativeIp: basestring | |
""" | |
nativeLine = vcfIp.split("\t") | |
somaticDict = {'0': 'Reference', '1': 'Germline', '2': 'Somatic', '3': 'LOH', '5': 'Unknown'} | |
chrom = nativeLine[0] | |
position = nativeLine[1] | |
ref = nativeLine[3] | |
var = nativeLine[4] | |
normalInfo = nativeLine[9] | |
tumorInfo = nativeLine[10] | |
normal_reads1 = normalInfo.split(":")[3] | |
normal_reads2 = normalInfo.split(":")[4] | |
normal_var_freq = normalInfo.split(":")[5] | |
normal_gt = normalInfo.split(":")[0] | |
normal_dp4 = normalInfo.split(":")[6] | |
normal_reads1_plus = normal_dp4.split(",")[0] | |
normal_reads1_minus = normal_dp4.split(",")[1] | |
normal_reads2_plus = normal_dp4.split(",")[2] | |
normal_reads2_minus = normal_dp4.split(",")[3] | |
tumor_reads1 = tumorInfo.split(":")[3] | |
tumor_reads2 = tumorInfo.split(":")[4] | |
tumor_var_freq = tumorInfo.split(":")[5] | |
tumor_gt = tumorInfo.split(":")[0] | |
tumor_dp4 = tumorInfo.split(":")[6] | |
tumor_reads1_plus = tumor_dp4.split(",")[0] | |
tumor_reads1_minus = tumor_dp4.split(",")[1] | |
tumor_reads2_plus = tumor_dp4.split(",")[2] | |
tumor_reads2_minus = tumor_dp4.split(",")[3] | |
info = nativeLine[7] | |
infoDict = {} | |
infoSpl = info.split(";") | |
for rec in infoSpl: | |
recSpl = rec.split("=") | |
if not len(recSpl) == 1: | |
infoDict[recSpl[0]] = recSpl[1] | |
somatic_status = somaticDict[infoDict['SS']] | |
variant_p_value = infoDict['GPV'] | |
somatic_p_value = infoDict['SPV'] | |
print("%s\t%s\t%s\t%s\t%s\t%s\t%s\t%s\t%s\t%s\t%s\t%s\t%s\t%s\t%s\t%s\t%s\t%s\t%s\t%s\t%s\t%s\t%s\t" % | |
(chrom, position, ref, var, normal_reads1, normal_reads2, normal_var_freq, normal_gt, tumor_reads1, | |
tumor_reads2, tumor_var_freq, tumor_gt, somatic_status, variant_p_value, somatic_p_value, tumor_reads1_plus, | |
tumor_reads1_minus, tumor_reads2_plus, tumor_reads2_minus, normal_reads1_plus, normal_reads1_minus, | |
normal_reads2_plus, normal_reads2_minus)) | |
##### | |
# Function to convert Native to VCF record | |
def makeVcfRecord(nativeIp): | |
""" | |
:rtype : Null | |
""" | |
somaticDict = {'Reference': '0', 'Germline': '1', 'Somatic': '2', 'LOH': '3', 'Unknown': '5'} | |
nIp = nativeIp.split("\t") | |
chrom = nIp[0] | |
pos = nIp[1] | |
id = '.' | |
ref = nIp[2] | |
alt = nIp[3] | |
qual = '.' | |
filter = 'PASS' | |
dp = int(nIp[4]) + int(nIp[5]) + int(nIp[8]) + int(nIp[9]) | |
ss = somaticDict[nIp[12]] | |
ssc = -10 * math.log10(float(nIp[14])) | |
gpv = nIp[13] | |
spv = nIp[14] | |
if ss == '2': | |
info = "DP=" + str(dp) + ";SOMATIC;" + "SS=" + ss + ";" + "SSC=" + str( | |
int(ssc)) + ";" + "GPV=" + gpv + ";" + "SPV=" + spv | |
else: | |
info = "DP=" + str(dp) + ";" + "SS=" + ss + ";" + "SSC=" + str( | |
int(ssc)) + ";" + "GPV=" + gpv + ";" + "SPV=" + spv | |
vcf_format = "GT:GQ:DP:RD:AD:FREQ:DP4" | |
normal_var_freq = float(re.sub("%", "", nIp[6])) | |
if normal_var_freq > 10 and normal_var_freq < 75: | |
gt = '0/1' | |
elif normal_var_freq > 75: | |
gt = '1/1' | |
else: | |
gt = "0/0" | |
tumor_var_freq = float(re.sub("%", "", nIp[10])) | |
if tumor_var_freq > 10 and tumor_var_freq < 75: | |
gt2 = '0/1' | |
elif tumor_var_freq > 75: | |
gt2 = '1/1' | |
else: | |
gt2 = "0/0" | |
gq = '.' | |
dp2 = int(nIp[4]) + int(nIp[5]) | |
rd = nIp[4] | |
ad = nIp[5] | |
freq = nIp[6] | |
dp4 = nIp[19] + ',' + nIp[20] + ',' + nIp[21] + ',' + nIp[22] | |
normal_format = gt + ':' + gq + ":" + str(dp2) + ':' + rd + ':' + ad + ':' + freq + ':' + dp4 | |
dp3 = int(nIp[8]) + int(nIp[9]) | |
rd2 = nIp[8] | |
ad2 = nIp[9] | |
freq2 = nIp[10] | |
dp42 = nIp[15] + ',' + nIp[16] + ',' + nIp[17] + ',' + nIp[19] | |
tumor_format = gt2 + ':' + gq + ":" + str(dp3) + ':' + rd2 + ':' + ad2 + ':' + freq2 + ':' + dp42 | |
print("%s\t%s\t%s\t%s\t%s\t%s\t%s\t%s\t%s\t%s\t%s" % | |
(chrom, pos, id, ref, alt, qual, filter, info, vcf_format, normal_format, tumor_format)) | |
#### | |
def NativeToVcf(inputFile): | |
printVcfHeader() | |
vs = open(inputFile, 'r') | |
for line in vs.readlines(): | |
if not line.startswith("chrom"): | |
makeVcfRecord(line.strip()) | |
vs.close() | |
### | |
def vcfToNative(inputFile): | |
vs = open(inputFile, 'r') | |
printNativeHeader() | |
for line in vs.readlines(): | |
if not line.startswith("#"): | |
makeNativeRec(line.strip()) | |
vs.close() | |
#### | |
vsIp = open(args.input, 'r') | |
firstLine = vsIp.readline().strip() | |
if firstLine.startswith("##fileformat="): | |
vcfToNative(args.input) | |
else: | |
NativeToVcf(args.input) | |
vsIp.close() |
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I download your new script and I get this error:
Traceback (most recent call last):
File "VarScan2_format_converter.py", line 212, in
NativeToVcf(args.input)
File "VarScan2_format_converter.py", line 191, in NativeToVcf
makeVcfRecord(line.strip())
File "VarScan2_format_converter.py", line 150, in makeVcfRecord
normal_var_freq = float(re.sub("%", "", nIp[6]))
ValueError: invalid literal for float(): 63,64