Mercurial > repos > miller-lab > genome_diversity
view make_phylip.py @ 31:a631c2f6d913
Update to Miller Lab devshed revision 3c4110ffacc3
| author | Richard Burhans <burhans@bx.psu.edu> |
|---|---|
| date | Fri, 20 Sep 2013 13:25:27 -0400 |
| parents | |
| children | ea52b23f1141 |
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#!/usr/bin/env python # -*- coding: utf-8 -*- # # mkFastas.py # # Copyright 2013 Oscar Reina <oscar@niska.bx.psu.edu> # # This program is free software; you can redistribute it and/or modify # it under the terms of the GNU General Public License as published by # the Free Software Foundation; either version 2 of the License, or # (at your option) any later version. # # This program is distributed in the hope that it will be useful, # but WITHOUT ANY WARRANTY; without even the implied warranty of # MERCHANTABILITY or FITNESS FOR A PARTICULAR PURPOSE. See the # GNU General Public License for more details. # # You should have received a copy of the GNU General Public License # along with this program; if not, write to the Free Software # Foundation, Inc., 51 Franklin Street, Fifth Floor, Boston, # MA 02110-1301, USA. import argparse import errno import os import shutil def mkdir_p(path): try: os.makedirs(path) except OSError, e: if e.errno <> errno.EEXIST: raise def revseq(seq): seq=list(seq) seq.reverse() seq=''.join(seq) return seq def revComp(allPop): dAllCompAll={'A':'T','T':'A','C':'G','G':'C','N':'N','M':'K','K':'M','R':'Y','Y':'R','W':'W','S':'S'} allPopsComp=dAllCompAll[allPop] return allPopsComp def rtrnCons(ntA,ntB): srtdPairs=''.join(sorted([ntA,ntB])) dpairsCons={'AC':'M', 'AG':'R', 'AT':'W', 'CG':'S', 'CT':'Y', 'GT':'K', 'AN':'A', 'CN':'C', 'GN':'G', 'NT':'T'} cons=dpairsCons[srtdPairs] return cons def rtrnFxdChrPos(inSNPf,dPopsinSNPfPos,pxchrx,pxpos,pxntA,pxntB,fulldChrdPosdPopsAlllsInit=False,cvrgTreshold=False,indvlsPrctTrshld=False): """ """ dChrdPosdPopsAlllsInit={} seqref=[] for eachl in open(inSNPf,'r'): if eachl.strip() and eachl[0]!='#': fllInfoSplt=eachl.splitlines()[0].split('\t') chrx=fllInfoSplt[pxchrx] pos=int(fllInfoSplt[pxpos]) ntA=fllInfoSplt[pxntA] ntB=fllInfoSplt[pxntB] seqref.append([pos,ntA]) dPopsAllls={} if fulldChrdPosdPopsAlllsInit: #~ cntIndv=0 # try: fulldPopsAllls=fulldChrdPosdPopsAlllsInit[chrx][pos] except: fulldPopsAllls=dict([(echPop,ntA) for echPop in dPopsinSNPfPos]) # for eachPop in dPopsinSNPfPos: clmnCvrg=dPopsinSNPfPos[eachPop] if clmnCvrg: eachPopCvrg=int(fllInfoSplt[clmnCvrg]) else: #~ eachPopCvrg=0 eachPopCvrg=cvrgTreshold if eachPopCvrg>=cvrgTreshold: dPopsAllls[eachPop]=fulldPopsAllls[eachPop] cntIndv+=1 else: dPopsAllls[eachPop]='N' #~ if indvlsPrctTrshld>(cntIndv/float(len(dPopsinSNPfPos))): dPopsAllls=dict([(echPop,'N') for echPop in dPopsinSNPfPos]) #~ else: for eachPop in dPopsinSNPfPos: if dPopsinSNPfPos[eachPop]: eachPopAll=int(fllInfoSplt[dPopsinSNPfPos[eachPop]]) if eachPopAll==0: dPopsAllls[eachPop]=ntB elif eachPopAll==2: dPopsAllls[eachPop]=ntA elif eachPopAll==1: dPopsAllls[eachPop]=rtrnCons(ntA,ntB) else: dPopsAllls[eachPop]='N' else: dPopsAllls[eachPop]=ntA try: dChrdPosdPopsAlllsInit[chrx][pos]=dPopsAllls except: dChrdPosdPopsAlllsInit[chrx]={pos:dPopsAllls} #~ seqref.sort() startExs=[seqref[0][0]] endExs=[seqref[-1][0]+1] seqref=''.join(x[1] for x in seqref) #~ return dChrdPosdPopsAlllsInit,seqref,chrx,startExs,endExs def rtrndENSEMBLTseq(inCDSfile,inUCSCfile,fchrClmn,txStartClmn,txEndClmn,strandClmn,geneNameClmn,startExsClmn,endExsClmn,cdsStartClmn,cdsEndClmn): """ """ dENSEMBLTchrxStEndEx={} dChrdStrtEndENSEMBLT={} for eachl in open(inUCSCfile,'r'): if eachl.strip(): rvrse=False allVls=eachl.split('\t') txStart=allVls[txStartClmn] txEnd=allVls[txEndClmn] ENSEMBLT=allVls[geneNameClmn] strand=allVls[strandClmn] chrx=allVls[fchrClmn] if cdsStartClmn and cdsEndClmn: cdsStart=allVls[cdsStartClmn] cdsEnd=allVls[cdsEndClmn] if startExsClmn and endExsClmn: startExs=allVls[startExsClmn] endExs=allVls[endExsClmn] if strand=='-': rvrse=True try: dChrdStrtEndENSEMBLT[chrx][int(txStart),int(txEnd)]=ENSEMBLT except: try: dChrdStrtEndENSEMBLT[chrx]={(int(txStart),int(txEnd)):ENSEMBLT} except: dChrdStrtEndENSEMBLT={chrx:{(int(txStart),int(txEnd)):ENSEMBLT}} #~ if cdsStartClmn and cdsEndClmn and startExsClmn and endExsClmn: startExs,endExs=rtrnExnStarEndCorrc(startExs,endExs,cdsStart,cdsEnd) else: startExs,endExs=[int(txStart)],[int(txEnd)] dENSEMBLTchrxStEndEx[ENSEMBLT]=(chrx,startExs,endExs,rvrse) #~ dENSEMBLTseq={} ENSEMBLTseqs=[(x.splitlines()[0],''.join(x.splitlines()[1:])) for x in open(inCDSfile).read().split('>') if x.strip()] for ENSEMBLT,seq in ENSEMBLTseqs: dENSEMBLTseq[ENSEMBLT]=seq #~ dENSEMBLTseqChrStEnEx={} for ENSEMBLT in dENSEMBLTchrxStEndEx: chrx,startExs,endExs,rvrse=dENSEMBLTchrxStEndEx[ENSEMBLT] addEseqChrStEnEx=True try: seq=dENSEMBLTseq[ENSEMBLT] if rvrse: seq=revseq(seq) except: addEseqChrStEnEx=False if addEseqChrStEnEx: dENSEMBLTseqChrStEnEx[ENSEMBLT]=(seq,chrx,startExs,endExs,rvrse) return dENSEMBLTseqChrStEnEx,dChrdStrtEndENSEMBLT def rtrnFxdChrPosinCodReg(dChrdStrtEndENSEMBLT,dChrdPosdPopsAlllsInit): """ """ dENSEMBLTChrPosdAlls={} dChrPosdPopsAllls={} todel=set(dChrdPosdPopsAlllsInit.keys()).difference(set(dChrdStrtEndENSEMBLT.keys())) for x in todel: x=dChrdPosdPopsAlllsInit.pop(x) #--- while len(dChrdPosdPopsAlllsInit)>0: chrx=dChrdPosdPopsAlllsInit.keys()[0] dStrtEndENSEMBLT=dChrdStrtEndENSEMBLT.pop(chrx) dPosdPopsAllls=dChrdPosdPopsAlllsInit.pop(chrx) #~ srtdStrtEndENSEMBLT=sorted(dStrtEndENSEMBLT.keys()) srtdPosdPopsAllls=sorted(dPosdPopsAllls.keys()) #~ pos=srtdPosdPopsAllls.pop(0) strt,end=srtdStrtEndENSEMBLT.pop(0) ENSEMBLT=dStrtEndENSEMBLT[strt,end] dPopsAllls=dPosdPopsAllls[pos] keePloop=True #~ while keePloop: if strt<=pos<=end: for tmpstrt,tmpend in [(strt,end)]+srtdStrtEndENSEMBLT: if tmpstrt<=pos<=tmpend: dPopsAllls=dPosdPopsAllls[pos] dChrPosdPopsAllls[chrx,pos]=dPopsAllls try: dENSEMBLTChrPosdAlls[ENSEMBLT][chrx,pos]=dPopsAllls except: dENSEMBLTChrPosdAlls[ENSEMBLT]={(chrx,pos):dPopsAllls} else: continue if len(srtdPosdPopsAllls)>0: pos=srtdPosdPopsAllls.pop(0) dPopsAllls=dPosdPopsAllls[pos] else: keePloop=False #~ elif pos<=strt: if len(srtdPosdPopsAllls)>0: pos=srtdPosdPopsAllls.pop(0) dPopsAllls=dPosdPopsAllls[pos] else: keePloop=False else: if len(srtdStrtEndENSEMBLT)>0: strt,end=srtdStrtEndENSEMBLT.pop(0) ENSEMBLT=dStrtEndENSEMBLT[strt,end] else: keePloop=False return dENSEMBLTChrPosdAlls,dChrPosdPopsAllls def rtrnExnStarEndCorrc(startExs,endExs,cdsStart,cdsEnd): """ """ cdsStart,cdsEnd=int(cdsStart),int(cdsEnd) crrctdstartExs=set([int(x) for x in startExs.split(',') if x.strip()]) crrctdendExs=set([int(x) for x in endExs.split(',') if x.strip()]) crrctdstartExs.add(cdsStart) crrctdendExs.add(cdsEnd) sStartDel=set() sEndDel=set() #~ for echvl in crrctdstartExs: if echvl<cdsStart or echvl>cdsEnd: sStartDel.add(echvl) #~ for echvl in crrctdendExs: if echvl<cdsStart or echvl>cdsEnd: sEndDel.add(echvl) #~ return sorted(crrctdstartExs.difference(sStartDel)),sorted(crrctdendExs.difference(sEndDel)) def rtrndPopsFasta(seq,chrx,startExs,endExs,rvrse,dChrPosdPopsAllls,ENSEMBLT): """ """ exnIntrvl=zip(startExs,endExs) CDSinitPos=exnIntrvl[0][0] dexnIntrvlSeq={} for exStart,exEnd in exnIntrvl: lenEx=exEnd-exStart dexnIntrvlSeq[exStart,exEnd]=seq[:lenEx] seq=seq[lenEx:] ldexnIntrvlSeq=len(dexnIntrvlSeq) #~ dPopsFasta={} #~ strePos=set() dStrePosAbsPos={} tmpAcmltdPos=0 #~ exStart,exEnd=sorted(dexnIntrvlSeq.keys())[0] seq=dexnIntrvlSeq.pop((exStart,exEnd)) chrx,pos=sorted(dChrPosdPopsAllls.keys())[0] dPopsAllls=dChrPosdPopsAllls.pop((chrx,pos)) tmpdPopsFasta=dict([(x,list(seq)) for x in dPopsAllls]) cntExns=0 while True: if exStart<=pos<=exEnd-1: relPos=tmpAcmltdPos+pos-exStart strePos.add(relPos) dStrePosAbsPos[relPos]=pos for echPop in tmpdPopsFasta: allPop=dPopsAllls[echPop] if rvrse: allPop=revComp(allPop) tmpdPopsFasta[echPop][pos-exStart]=allPop if len(dChrPosdPopsAllls)>0: chrx,pos=sorted(dChrPosdPopsAllls.keys())[0] dPopsAllls=dChrPosdPopsAllls.pop((chrx,pos)) else: pos=endExs[-1]+100#max pos of exns elif pos<exStart: if len(dChrPosdPopsAllls)>0: chrx,pos=sorted(dChrPosdPopsAllls.keys())[0] dPopsAllls=dChrPosdPopsAllls.pop((chrx,pos)) else: pos=endExs[-1]+100#max pos of exns elif pos>exEnd-1:# or len(dChrPosdPopsAllls)==0: for echPop in tmpdPopsFasta: try: dPopsFasta[echPop]+=''.join(tmpdPopsFasta[echPop]) except: dPopsFasta[echPop]=''.join(tmpdPopsFasta[echPop]) cntExns+=1 tmpAcmltdPos+=len(seq) if len(dexnIntrvlSeq)>0: exStart,exEnd=sorted(dexnIntrvlSeq.keys())[0] seq=dexnIntrvlSeq.pop((exStart,exEnd)) tmpdPopsFasta=dict([(x,list(seq)) for x in dPopsAllls]) else: break if ldexnIntrvlSeq!=cntExns: for echPop in tmpdPopsFasta: dPopsFasta[echPop]+=''.join(tmpdPopsFasta[echPop]) #~ lchrStartexEndpos=[] if rvrse: dPopsFasta=dict([(echPop,revseq(dPopsFasta[echPop])) for echPop in dPopsFasta])#[echPop]+=''.join(tmpdPopsFasta[echPop]) for ePos in strePos: lchrStartexEndpos.append('\t'.join([ENSEMBLT,chrx,str(tmpAcmltdPos-ePos-1),str(dStrePosAbsPos[ePos])])) else: for ePos in strePos: lchrStartexEndpos.append('\t'.join([ENSEMBLT,chrx,str(ePos),str(dStrePosAbsPos[ePos])])) #~ return dPopsFasta,lchrStartexEndpos def rtrnSeqVars(dENSEMBLTseqChrStEnEx,dENSEMBLTChrPosdAlls): """ """ dENSEMBLTPopsFasta={} lchrStartexEndposAll=[] #~ sENSEMBLTcmmn=set(dENSEMBLTChrPosdAlls.keys()).intersection(set(dENSEMBLTseqChrStEnEx.keys()))#sENSEMBLTcmmn between UCSC and ENSEMBLE #~ for ENSEMBLT in sENSEMBLTcmmn: seq,chrx,startExs,endExs,rvrse=dENSEMBLTseqChrStEnEx[ENSEMBLT] dChrPosdPopsAllls=dENSEMBLTChrPosdAlls[ENSEMBLT] if len(startExs)>0 and len(endExs)>0: dPopsFasta,lchrStartexEndpos=rtrndPopsFasta(seq,chrx,startExs,endExs,rvrse,dChrPosdPopsAllls,ENSEMBLT) lchrStartexEndposAll.extend(lchrStartexEndpos) if dPopsFasta:#to correct a bug of the input table, in cases in which endExons<startExn (!). See ENSCAFT00000000145 (MC4R) in canFam2 for example. dENSEMBLTPopsFasta[ENSEMBLT]=dPopsFasta return dENSEMBLTPopsFasta,lchrStartexEndposAll def rtrnPhy(dPopsFasta,ENSEMBLT): """ """ dPopsFormPhy={} for eachPop in dPopsFasta: hader='%s'%eachPop #~ hader='>%s'%eachPop seq=dPopsFasta[eachPop] formtd='\t'.join([hader,seq]) #~ formtd='\n'.join([hader,seq]) dPopsFormPhy[eachPop]=formtd #~ return dPopsFormPhy,len(seq) def wrapSeqsFasta(dENSEMBLTPopsFasta,outFastaFold,sPopsIntrst): """ """ ENSEMBLTKaKs=[] nonHeader=True cnt=0 lENSEMBLT=len(dENSEMBLTPopsFasta) #~ for ENSEMBLT in sorted(dENSEMBLTPopsFasta.keys()): cnt+=1 dPopsFasta=dENSEMBLTPopsFasta[ENSEMBLT] dPopsFormPhy,lenseq=rtrnPhy(dPopsFasta,ENSEMBLT) #~ seqPMLformat=['%s %s'%(len(dPopsFormPhy),lenseq)]#generate new PHYML sequence #~ seqPMLformat=[]#generate new PHYML sequence for namex in sorted(sPopsIntrst): seqPMLformat.append(dPopsFormPhy[namex]) #~ mkdir_p(outFastaFold) outFastaf=os.path.join(outFastaFold,'%s.phy'%ENSEMBLT) outFastaf=open(outFastaf,'w') outFastaf.write('\n'.join(seqPMLformat)) outFastaf.close() #~ return 0 def main(): #~ #~bpython mkPhyl.py --input=colugo_mt_Galaxy_genotypes.txt --chrClmn=0 --posClmn=1 --refClmn=2 --altrClmn=3 --output=out.d --gd_indivs=genotypes.gd_indivs --inputCover=colugo_mt_Galaxy_coverage.txt --gd_indivs_cover=coverage.gd_indivs --cvrgTreshold=0 --chrClmnCvrg=0 --posClmnCvrg=1 --refClmnCvrg=2 --altrClmnCvrg=3 --indvlsPrctTrshld=0 parser = argparse.ArgumentParser(description='Returns the count of genes in KEGG categories and their statistical overrrepresentation, from a list of genes and an background file (i.e. plane text with ENSEMBLT and KEGG pathways).') parser.add_argument('--input',metavar='input gd_snp file',type=str,help='the input file with the table in gd_snp/gd_genotype format.',required=True) parser.add_argument('--chrClmn',metavar='int',type=int,help='the column with the chromosome.',required=True) parser.add_argument('--posClmn',metavar='int',type=int,help='the column with the SNPs position.',required=True) parser.add_argument('--refClmn',metavar='int',type=int,help='the column with the reference nucleotide.',required=True) parser.add_argument('--altrClmn',metavar='int',type=int,help='the column with the derived nucleotide.',required=True) parser.add_argument('--output',metavar='output',type=str,help='the output',required=True) parser.add_argument('--output_id',metavar='int',type=int,help='the output id',required=True) parser.add_argument('--output_dir',metavar='output folder sequences',type=str,help='the output folder with the sequences.',required=True) parser.add_argument('--gd_indivs',metavar='input gd_indivs file',type=str,help='the input reference species columns in the input file.',required=True) #~ parser.add_argument('--inputCover',metavar='input gd_snp cover file',type=str,help='the input file with the table in gd_snp/gd_genotype cover format.',required=False,default=False) parser.add_argument('--gd_indivs_cover',metavar='input gd_indivs file',type=str,help='the input reference species columns in the input cover file.',required=False,default=False) parser.add_argument('--cvrgTreshold',metavar='input coverage threshold',type=int,help='the coverage threshold above which nucleotides are included, else "N".',required=False,default=False) parser.add_argument('--chrClmnCvrg',metavar='int',type=int,help='the column with the chromosome in the input coverage file.',required=False,default=False) parser.add_argument('--posClmnCvrg',metavar='int',type=int,help='the column with the SNPs position in the input coverage file.',required=False,default=False) parser.add_argument('--refClmnCvrg',metavar='int',type=int,help='the column with the reference nucleotide in the input coverage file.',required=False,default=False) parser.add_argument('--altrClmnCvrg',metavar='int',type=int,help='the column with the derived nucleotide in the input coverage file.',required=False,default=False) parser.add_argument('--indvlsPrctTrshld',metavar='int',type=float,help='the percentage of individual above which nucleotides are included, else "N".',required=False,default=False) #~ parser.add_argument('--sequence',metavar='input fasta file',type=str,help='the input file with the sequence whose SNPs are in the input.',required=False,default=False) parser.add_argument('--gene_info',metavar='input interval file',type=str,help='the input interval file with the the information on the genes.',required=False,default=False) parser.add_argument('--fchrClmn',metavar='int',type=int,help='the column with the chromosome in the gene_info file.',required=False,default=False) parser.add_argument('--txStartClmn',metavar='int',type=int,help='the column with the transcript start column in the gene_info file.',required=False,default=False) parser.add_argument('--txEndClmn',metavar='int',type=int,help='the column with the transcript end column in the gene_info file.',required=False,default=False) parser.add_argument('--strandClmn',metavar='int',type=int,help='the column with the strand column in the gene_info file.',required=False,default=False) parser.add_argument('--geneNameClmn',metavar='int',type=int,help='the column with the gene name column in the gene_info file.',required=False,default=False) parser.add_argument('--cdsStartClmn',metavar='int',type=int,help='the column with the coding start column in the gene_info file.',required=False,default=False) parser.add_argument('--cdsEndClmn',metavar='int',type=int,help='the column with the coding end column in the gene_info file.',required=False,default=False) parser.add_argument('--startExsClmn',metavar='int',type=int,help='the column with the exon start positions column in the gene_info file.',required=False,default=False) parser.add_argument('--endExsClmn',metavar='int',type=int,help='the column with the exon end positions column in the gene_info file.',required=False,default=False) args = parser.parse_args() inSNPf = args.input outfile = args.output outfile_id = args.output_id outFastaFold = './out' files_dir = args.output_dir gd_indivs = args.gd_indivs pxchrx = args.chrClmn pxpos = args.posClmn pxntA = args.refClmn pxntB = args.altrClmn inCDSfile = args.sequence inUCSCfile = args.gene_info fchrClmn = args.fchrClmn#chromosome column txStartClmn = args.txStartClmn#transcript start column txEndClmn = args.txEndClmn#transcript end column strandClmn = args.strandClmn#strand column geneNameClmn = args.geneNameClmn#gene name column cdsStartClmn = args.cdsStartClmn#coding sequence start column cdsEndClmn = args.cdsEndClmn#coding sequence end column startExsClmn = args.startExsClmn#exons start column endExsClmn = args.endExsClmn#exons end column inputCover = args.inputCover gd_indivs_cover = args.gd_indivs_cover cvrgTreshold = args.cvrgTreshold pxchrxCov = args.chrClmnCvrg pxposCov = args.posClmnCvrg pxntACov = args.refClmnCvrg pxntBCov = args.altrClmnCvrg indvlsPrctTrshld = args.indvlsPrctTrshld #print inputCover, gd_indivs_cover, cvrgTreshold assert ((inputCover and gd_indivs_cover and cvrgTreshold>=0 and indvlsPrctTrshld>=0) or (inCDSfile and inUCSCfile)) #~ dPopsinSNPfPos=dict([(x.split()[1],int(x.split()[0])-1) for x in open(gd_indivs).read().splitlines() if x.strip()]) #~ dPopsinSNPfPos.update({'ref':False}) #~ sPopsIntrst=set(dPopsinSNPfPos.keys()) dChrdPosdPopsAlllsInit,seqref,chrx,startExs,endExs=rtrnFxdChrPos(inSNPf,dPopsinSNPfPos,pxchrx,pxpos,pxntA,pxntB)#~ print '1. Getting fixed alleles information...' #~ dENSEMBLTseqChrStEnEx,dChrdStrtEndENSEMBLT=rtrndENSEMBLTseq(inCDSfile,inUCSCfile) #~ if inputCover and gd_indivs_cover and cvrgTreshold>=0: dPopsinSNPfPos_cover=dict([(eachPop,False) for eachPop in dPopsinSNPfPos.keys()]) dPopsinSNPfPos_cover.update(dict([(x.split()[1],int(x.split()[0])-1) for x in open(gd_indivs_cover).read().splitlines() if x.strip()])) dChrdPosdPopsAlllsInit,seqref,chrx,startExs,endExs=rtrnFxdChrPos(inputCover,dPopsinSNPfPos_cover,pxchrxCov,pxposCov,pxntACov,pxntBCov,dChrdPosdPopsAlllsInit,cvrgTreshold,indvlsPrctTrshld) rvrse=False dENSEMBLTseqChrStEnEx={'tmp':(seqref,chrx,startExs,endExs,rvrse)} dChrdStrtEndENSEMBLT={chrx:{(startExs[0],endExs[0]):'tmp'}} #~ elif inCDSfile and inUCSCfile: dENSEMBLTseqChrStEnEx,dChrdStrtEndENSEMBLT=rtrndENSEMBLTseq(inCDSfile,inUCSCfile,fchrClmn,txStartClmn,txEndClmn,strandClmn,geneNameClmn,startExsClmn,endExsClmn,cdsStartClmn,cdsEndClmn)#~ print '2. Getting transcripts and exons information...' #~ dENSEMBLTChrPosdAlls,dChrPosdPopsAllls=rtrnFxdChrPosinCodReg(dChrdStrtEndENSEMBLT,dChrdPosdPopsAlllsInit)#~ print '3. Getting fixed alleles in exons...' #~ dENSEMBLTPopsFasta,lchrStartexEndposAll=rtrnSeqVars(dENSEMBLTseqChrStEnEx,dENSEMBLTChrPosdAlls)#~ print '4. Getting fasta sequences of populations...' #~ wrapSeqsFasta(dENSEMBLTPopsFasta,outFastaFold,sPopsIntrst) #~ ## get a lit of output files files = [] for dirpath, dirnames, filenames in os.walk(outFastaFold): for file in filenames: if file.endswith('.phy'): files.append( os.path.join(dirpath, file) ) del dirnames[:] if len(files) == 0: with open(outfile, 'w') as ofh: print >> ofh, 'No output.' else: ## the first file becomes the output file = files.pop(0) shutil.move(file, outfile) ## rename/move the rest of the files for i, file in enumerate(files): new_filename = 'primary_{0}_output{1}_visible_txt_?'.format(outfile_id, i+2) new_pathname = os.path.join(files_dir, new_filename) shutil.move(file, new_pathname) return 0 if __name__ == '__main__': main()