Mercurial > repos > miller-lab > snp_analysis_conversion
view gd_snp2vcf.pl @ 3:edf12470a1a6 default tip
Bugfix from Belinda, in vcf2pgSnp.pl
author | Cathy Riemer <cathy+hg@bx.psu.edu> |
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date | Thu, 19 Mar 2015 12:06:34 -0400 |
parents | 35c20b109be5 |
children |
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#!/usr/bin/perl -w use strict; #convert from gd_snp file to vcf file (with dbSNP fields) #gd_snp table format: #1. chr #2. position (0 based) #3. ref allele #4. second allele #5. overall quality #foreach individual (6-9, 10-13, ...) #a. count of allele in 3 #b. count of allele in 4 #c. genotype call (-1, or count of ref allele) #d. quality of genotype call (quality of non-ref allele from masterVar) if (!@ARGV) { print "usage: gd_snp2vcf.pl file.gd_snp[.gz|.bz2] -geno=8[,12:16,20...] -handle=HANDLE -batch=BATCHNAME -ref=REFERENCEID [-bioproj=XYZ -biosamp=ABC -pop=POPID[,POPID2...] -chrCol=9 -posCol=9 ] > snpsForSubmission.vcf\n"; exit; } my $in = shift @ARGV; my $genoCols = ''; my $handle; my $batch; my $bioproj; my $biosamp; my $ref; my $pop; my $cr = 0; #allow to use alternate reference? my $cp = 1; my $meta; foreach (@ARGV) { if (/-geno=([0-9,]+)/) { $genoCols .= "$1:"; } elsif (/-handle=(.*)/) { $handle = $1; } elsif (/-batch=(.*)/) { $batch = $1; } elsif (/-bioproj=(.*)/) { $bioproj = $1; } elsif (/-biosamp=(.*)/) { $biosamp = $1; } elsif (/-ref=(.*)/) { $ref = $1; } elsif (/-population=(\S+)/) { $pop = $1; } elsif (/-chrCol=(\d+)/) { $cr = $1 - 1; } elsif (/-posCol=(\d+)/) { $cp = $1 - 1; } elsif (/-metaOut=(.*)/) { $meta = $1; } } if ($cr < 0 or $cp < 0) { die "ERROR the column numbers should be 1 based.\n"; } #remove trailing delimiters $genoCols =~ s/,:/:/g; $genoCols =~ s/[,:]$//; my @gnc = split(/,|:/, $genoCols); if ($in =~ /.gz$/) { open(FH, "zcat $in |") or die "Couldn't open $in, $!\n"; }elsif ($in =~ /.bz2$/) { open(FH, "bzcat $in |") or die "Couldn't open $in, $!\n"; }else { open(FH, $in) or die "Couldn't open $in, $!\n"; } my @head = prepHeader(); if (@head) { print join("\n", @head), "\n"; #now column headers print "#CHROM\tPOS\tID\tREF\tALT\tQUAL\tFILTER\tINFO"; if (defined $pop) { $pop =~ s/,$//; my $t = $pop; $t =~ s/,/\t/g; print "\tFORMAT\t$t"; } print "\n"; } while (<FH>) { chomp; if (/^#/) { next; } if (/^\s*$/) { next; } my @f = split(/\t/); #vcf columns: chrom pos id ref alt qual filter info # info must have VRT=[0-9] 1==SNV 2=indel 6=NoVariation 8=MNV ... my $vrt = 1; if ($f[2] !~ /^[ACTG]$/ or $f[3] !~ /^[ACTG]$/) { die "Sorry this can only do SNV's at this time\n"; } if (scalar @gnc == 1) { #single genotype column if (!defined $f[4] or $f[4] == -1) { $f[4] = '.'; } if ($f[$gnc[0]-1] == 2) { $vrt = 6; } #reference match print "$f[$cr]\t$f[$cp]\t$f[$cr];$f[$cp]\t$f[2]\t$f[3]\t$f[4]\t.\tVRT=$vrt\n"; #TODO? put read counts in comment? }elsif ($pop) { #do as population my @cols; foreach my $gp (split(/:/,$genoCols)) { #foreach population my @g = split(/,/, $gp); my $totChrom = 2*(scalar @g); my $totRef = 0; foreach my $i (@g) { if ($f[$i-1] == -1) { next; } $totRef += $f[$i-1]; } if ($totChrom == $totRef) { $vrt = 6; } if ($totRef > $totChrom) { die "ERROR likely the wrong column was chosen for genotype\n"; } my $altCnt = $totChrom - $totRef; push(@cols, "$totChrom:$altCnt"); } print "$f[$cr]\t$f[$cp]\t$f[$cr];$f[$cp]\t$f[2]\t$f[3]\t$f[4]\t.\tVRT=$vrt\tNA:AC\t", join("\t", @cols), "\n"; }else { #leave allele counts off my $totChrom = 2*(scalar @gnc); my $totRef = 0; foreach my $i (@gnc) { if ($f[$i-1] == -1) { next; } $totRef += $f[$i-1]; } if ($totChrom == $totRef) { $vrt = 6; } print "$f[$cr]\t$f[$cp]\t$f[$cr];$f[$cp]\t$f[2]\t$f[3]\t$f[4]\t.\tVRT=$vrt\n"; } } close FH or die "Couldn't close $in, $!\n"; if ($meta) { open(FH, ">", $meta) or die "Couldn't open $meta, $!\n"; print FH "TYPE: CONT\n", "HANDLE: $handle\n", "NAME: \n", "FAX: \n", "TEL: \n", "EMAIL: \n", "LAB: \n", "INST: \n", "ADDR: \n", "||\n", "TYPE: METHOD\n", "HANDLE: $handle\n", "ID: \n", "METHOD_CLASS: Sequence\n", "TEMPLATE_TYPE: \n", "METHOD:\n", "||\n"; if ($pop) { my @p = split(/,/, $pop); foreach my $t (@p) { print FH "TYPE: POPULATION\n", "HANDLE: $handle\n", "ID: $t\n", "POPULATION: \n", "||\n"; } } print FH "TYPE: SNPASSAY\n", "HANDLE: $handle\n", "BATCH: $batch\n", "MOLTYPE: \n", "METHOD: \n", "ORGANISM: \n", "||\n", "TYPE: SNPPOPUSE | SNPINDUSE\n", "HANDLE: $handle\n", "BATCH: \n", "METHOD: \n", "||\n"; close FH or die "Couldn't close $meta, $!\n"; } exit 0; #parse old header and add or create new sub prepHeader { my @h; $h[0] = '##fileformat=VCFv4.1'; my ($day, $mo, $yr) = (localtime)[3,4,5]; $mo++; $yr+=1900; $h[1] = '##fileDate=' . "$yr$mo$day"; $h[2] = "##handle=$handle"; $h[3] = "##batch=$batch"; my $i = 4; if ($bioproj) { $h[$i] = "##bioproject_id=$bioproj"; $i++; } if ($biosamp) { $h[$i] = "##biosample_id=$biosamp"; $i++; } $h[$i] = "##reference=$ref"; ##reference=GCF_999999.99 #$i++; #$h[$i] = '##INFO=<ID=LID, Number=1,Type=string, Description="Unique local variation ID or name for display. The LID provided here combined with the handle must be unique for a particular submitter.">' $i++; $h[$i] = '##INFO=<ID=VRT,Number=1,Type=Integer,Description="Variation type,1 - SNV: single nucleotide variation,2 - DIV: deletion/insertion variation,3 - HETEROZYGOUS: variable, but undefined at nucleotide level,4 - STR: short tandem repeat (microsatellite) variation, 5 - NAMED: insertion/deletion variation of named repetitive element,6 - NO VARIATON: sequence scanned for variation, but none observed,7 - MIXED: cluster contains submissions from 2 or more allelic classes (not used) ,8 - MNV: multiple nucleotide variation with all eles of common length greater than 1,9 - Exception">'; #sometimes have allele freqs? if (defined $pop) { $i++; $h[$i] = "##FORMAT=<ID=NA,Number=1,Type=Integer,Description=\"Number of alleles for the population.\""; $i++; $h[$i] = '##FORMAT=<ID=AC,Number=.,Type=Integer,Description="Allele count for each alternate allele.">'; my @p = split(/,/, $pop); foreach my $t (@p) { $i++; $h[$i] = "##population_id=$t"; } } #PMID? ##INFO=<ID=PMID,Number=.,Type=Integer,Description="PubMed ID linked to variation if available."> return @h; } ####End