retrieve_ensembl_bed: bedutil.py comparison

comparison bedutil.py @ 0:da1b538b87e5 draft

planemo upload for repository https://github.com/galaxyproteomics/tools-galaxyp/tree/master/tools/proteogenomics/retrieve_ensembl_bed commit 88cf1e923a8c9e5bc6953ad412d15a7c70f054d1

author	galaxyp
date	Mon, 22 Jan 2018 13:13:47 -0500
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children

comparison

equal deleted inserted replaced

--1:000000000000
+:da1b538b87e5
+#!/usr/bin/env python
+"""
+#
+#------------------------------------------------------------------------------
+#                         University of Minnesota
+#         Copyright 2016, Regents of the University of Minnesota
+#------------------------------------------------------------------------------
+# Author:
+#
+#  James E Johnson
+#
+#------------------------------------------------------------------------------
+"""
+from __future__ import print_function
+import sys
+from Bio.Seq import reverse_complement, translate
+def bed_from_line(line, ensembl=False, seq_column=None):
+fields = line.rstrip('\r\n').split('\t')
+if len(fields) < 12:
+return None
+(chrom, chromStart, chromEnd, name, score, strand,
+thickStart, thickEnd, itemRgb,
+blockCount, blockSizes, blockStarts) = fields[0:12]
+bed_entry = BedEntry(chrom=chrom, chromStart=chromStart, chromEnd=chromEnd,
+name=name, score=score, strand=strand,
+thickStart=thickStart, thickEnd=thickEnd,
+itemRgb=itemRgb,
+blockCount=blockCount,
+blockSizes=blockSizes.rstrip(','),
+blockStarts=blockStarts.rstrip(','))
+if seq_column is not None and -len(fields) <= seq_column < len(fields):
+bed_entry.seq = fields[seq_column]
+if ensembl and len(fields) >= 20:
+bed_entry.second_name = fields[12]
+bed_entry.cds_start_status = fields[13]
+bed_entry.cds_end_status = fields[14]
+bed_entry.exon_frames = fields[15].rstrip(',')
+bed_entry.biotype = fields[16]
+bed_entry.gene_name = fields[17]
+bed_entry.second_gene_name = fields[18]
+bed_entry.gene_type = fields[19]
+return bed_entry
+def as_int_list(obj):
+if obj is None:
+return None
+if isinstance(obj, list):
+return [int(x) for x in obj]
+elif isinstance(obj, str):
+return [int(x) for x in obj.split(',')]
+else:  # python2 unicode?
+return [int(x) for x in str(obj).split(',')]
+class BedEntry(object):
+def __init__(self, chrom=None, chromStart=None, chromEnd=None,
+name=None, score=None, strand=None,
+thickStart=None, thickEnd=None, itemRgb=None,
+blockCount=None, blockSizes=None, blockStarts=None):
+self.chrom = chrom
+self.chromStart = int(chromStart)
+self.chromEnd = int(chromEnd)
+self.name = name
+self.score = int(score) if score is not None else 0
+self.strand = '-' if str(strand).startswith('-') else '+'
+self.thickStart = int(thickStart) if thickStart else self.chromStart
+self.thickEnd = int(thickEnd) if thickEnd else self.chromEnd
+self.itemRgb = str(itemRgb) if itemRgb is not None else r'100,100,100'
+self.blockCount = int(blockCount)
+self.blockSizes = as_int_list(blockSizes)
+self.blockStarts = as_int_list(blockStarts)
+self.second_name = None
+self.cds_start_status = None
+self.cds_end_status = None
+self.exon_frames = None
+self.biotype = None
+self.gene_name = None
+self.second_gene_name = None
+self.gene_type = None
+self.seq = None
+self.cdna = None
+self.pep = None
+# T26C
+self.aa_change = []
+# p.Trp26Cys g.<pos><ref>><alt> # g.1304573A>G
+self.variants = []
+def __str__(self):
+return '%s\t%d\t%d\t%s\t%d\t%s\t%d\t%d\t%s\t%d\t%s\t%s' % (
+self.chrom, self.chromStart, self.chromEnd,
+self.name, self.score, self.strand,
+self.thickStart, self.thickEnd, str(self.itemRgb), self.blockCount,
+','.join([str(x) for x in self.blockSizes]),
+','.join([str(x) for x in self.blockStarts]))
+def get_splice_junctions(self):
+splice_juncs = []
+for i in range(self.blockCount - 1):
+splice_junc = "%s:%d_%d"\
+% (self.chrom,
+self.chromStart + self.blockSizes[i],
+self.chromStart + self.blockStarts[i+1])
+splice_juncs.append(splice_junc)
+return splice_juncs
+def get_exon_seqs(self):
+if not self.seq:
+return None
+exons = []
+for i in range(self.blockCount):
+exons.append(self.seq[self.blockStarts[i]:self.blockStarts[i]
++ self.blockSizes[i]])
+if self.strand == '-':  # reverse complement
+exons.reverse()
+for i, s in enumerate(exons):
+exons[i] = reverse_complement(s)
+return exons
+def get_spliced_seq(self, strand=None):
+if not self.seq:
+return None
+seq = ''.join(self.get_exon_seqs())
+if strand and self.strand != strand:
+seq = reverse_complement(seq)
+return seq
+def get_cdna(self):
+if not self.cdna:
+self.cdna = self.get_spliced_seq()
+return self.cdna
+def get_cds(self):
+cdna = self.get_cdna()
+if cdna:
+if self.chromStart == self.thickStart\
+and self.chromEnd == self.thickEnd:
+return cdna
+pos = [self.cdna_offset_of_pos(self.thickStart),
+self.cdna_offset_of_pos(self.thickEnd)]
+if 0 <= min(pos) <= max(pos) <= len(cdna):
+return cdna[min(pos):max(pos)]
+return None
+def set_cds(self, cdna_start, cdna_end):
+cdna_len = sum(self.blockSizes)
+if 0 <= cdna_start < cdna_end <= cdna_len:
+cds_pos = [self.pos_of_cdna_offet(cdna_start),
+self.pos_of_cdna_offet(cdna_end)]
+if all(cds_pos):
+self.thickStart = min(cds_pos)
+self.thickEnd = max(cds_pos)
+return self
+return None
+def trim_cds(self, basepairs):
+if self.chromStart <= self.thickStart < self.thickEnd <= self.chromEnd:
+cds_pos = [self.cdna_offset_of_pos(self.thickStart),
+self.cdna_offset_of_pos(self.thickEnd)]
+if basepairs > 0:
+return self.set_cds(min(cds_pos) + basepairs, max(cds_pos))
+else:
+return self.set_cds(min(cds_pos), max(cds_pos) + basepairs)
+return None
+def get_cds_bed(self):
+cds_pos = [self.cdna_offset_of_pos(self.thickStart),
+self.cdna_offset_of_pos(self.thickEnd)]
+return self.trim(min(cds_pos), max(cds_pos))
+def get_cigar(self):
+cigar = ''
+r = range(self.blockCount)
+xl = None
+for x in r:
+if xl is not None:
+intronSize = abs(self.blockStarts[x] - self.blockSizes[xl]
+- self.blockStarts[xl])
+cigar += '%dN' % intronSize
+cigar += '%dM' % self.blockSizes[x]
+xl = x
+return cigar
+def get_cigar_md(self):
+cigar = ''
+md = ''
+r = range(self.blockCount)
+xl = None
+for x in r:
+if xl is not None:
+intronSize = abs(self.blockStarts[x] - self.blockSizes[xl]
+- self.blockStarts[xl])
+cigar += '%dN' % intronSize
+cigar += '%dM' % self.blockSizes[x]
+xl = x
+md = '%d' % sum(self.blockSizes)
+return (cigar, md)
+def get_translation(self, sequence=None):
+translation = None
+seq = sequence if sequence else self.get_spliced_seq()
+if seq:
+seqlen = len(seq) / 3 * 3
+if seqlen >= 3:
+translation = translate(seq[:seqlen])
+return translation
+def get_translations(self):
+translations = []
+seq = self.get_spliced_seq()
+if seq:
+for i in range(3):
+translation = self.get_translation(sequence=seq[i:])
+if translation:
+translations.append(translation)
+return translations
+def pos_of_cdna_offet(self, offset):
+if offset is not None and 0 <= offset < sum(self.blockSizes):
+r = list(range(self.blockCount))
+rev = self.strand == '-'
+if rev:
+r.reverse()
+nlen = 0
+for x in r:
+if offset < nlen + self.blockSizes[x]:
+if rev:
+return self.chromStart + self.blockStarts[x]\
++ self.blockSizes[x] - (offset - nlen)
+else:
+return self.chromStart + self.blockStarts[x]\
++ (offset - nlen)
+nlen += self.blockSizes[x]
+return None
+def cdna_offset_of_pos(self, pos):
+if not self.chromStart <= pos < self.chromEnd:
+return -1
+r = list(range(self.blockCount))
+rev = self.strand == '-'
+if rev:
+r.reverse()
+nlen = 0
+for x in r:
+bStart = self.chromStart + self.blockStarts[x]
+bEnd = bStart + self.blockSizes[x]
+if bStart <= pos < bEnd:
+return nlen + (bEnd - pos if rev else pos - bStart)
+nlen += self.blockSizes[x]
+def apply_variant(self, pos, ref, alt):
+pos = int(pos)
+if not ref or not alt:
+print("variant requires ref and alt sequences", file=sys.stderr)
+return
+if not self.chromStart <= pos <= self.chromEnd:
+print("variant not in entry %s: %s %d < %d < %d" %
+(self.name, self.strand,
+self.chromStart, pos, self.chromEnd),
+file=sys.stderr)
+print("%s" % str(self), file=sys.stderr)
+return
+if len(ref) != len(alt):
+print("variant only works for snp: %s  %s" % (ref, alt),
+file=sys.stderr)
+return
+if not self.seq:
+print("variant entry %s has no seq" % self.name, file=sys.stderr)
+return
+"""
+if self.strand  == '-':
+ref = reverse_complement(ref)
+alt = reverse_complement(alt)
+"""
+bases = list(self.seq)
+offset = pos - self.chromStart
+for i in range(len(ref)):
+# offset = self.cdna_offset_of_pos(pos+i)
+if offset is not None:
+bases[offset+i] = alt[i]
+else:
+print("variant offset %s: %s %d < %d < %d" %
+(self.name, self.strand, self.chromStart,
+pos+1, self.chromEnd), file=sys.stderr)
+print("%s" % str(self), file=sys.stderr)
+self.seq = ''.join(bases)
+self.variants.append("g.%d%s>%s" % (pos+1, ref, alt))
+def get_variant_bed(self, pos, ref, alt):
+pos = int(pos)
+if not ref or not alt:
+print("variant requires ref and alt sequences", file=sys.stderr)
+return None
+if not self.chromStart <= pos <= self.chromEnd:
+print("variant not in entry %s: %s %d < %d < %d" %
+(self.name, self.strand,
+self.chromStart, pos, self.chromEnd),
+file=sys.stderr)
+print("%s" % str(self), file=sys.stderr)
+return None
+if not self.seq:
+print("variant entry %s has no seq" % self.name, file=sys.stderr)
+return None
+tbed = BedEntry(chrom=self.chrom,
+chromStart=self.chromStart, chromEnd=self.chromEnd,
+name=self.name, score=self.score, strand=self.strand,
+thickStart=self.chromStart, thickEnd=self.chromEnd,
+itemRgb=self.itemRgb,
+blockCount=self.blockCount,
+blockSizes=self.blockSizes,
+blockStarts=self.blockStarts)
+bases = list(self.seq)
+offset = pos - self.chromStart
+tbed.seq = ''.join(bases[:offset] + list(alt)
++ bases[offset+len(ref):])
+if len(ref) != len(alt):
+diff = len(alt) - len(ref)
+rEnd = pos + len(ref)
+# need to adjust blocks
+#  change spans blocks,
+for x in range(tbed.blockCount):
+bStart = tbed.chromStart + tbed.blockStarts[x]
+bEnd = bStart + tbed.blockSizes[x]
+# change within a block or extends (last block)
+#  adjust blocksize
+#  seq:            GGGcatGGG
+#  ref c alt tag:  GGGtagatGGG
+#  ref cat alt a:  GGGaGGG
+if bStart <= pos < rEnd < bEnd:
+tbed.blockSizes[x] += diff
+return tbed
+# (start, end)
+def get_subrange(self, tstart, tstop, debug=False):
+chromStart = self.chromStart
+chromEnd = self.chromEnd
+if debug:
+print("%s" % (str(self)), file=sys.stderr)
+r = list(range(self.blockCount))
+if self.strand == '-':
+r.reverse()
+bStart = 0
+bEnd = 0
+for x in r:
+bEnd = bStart + self.blockSizes[x]
+if bStart <= tstart < bEnd:
+if self.strand == '+':
+chromStart = self.chromStart + self.blockStarts[x] +\
+(tstart - bStart)
+else:
+chromEnd = self.chromStart + self.blockStarts[x] +\
+self.blockSizes[x] - (tstart - bStart)
+if bStart <= tstop < bEnd:
+if self.strand == '+':
+chromEnd = self.chromStart + self.blockStarts[x] +\
+(tstop - bStart)
+else:
+chromStart = self.chromStart + self.blockStarts[x] +\
+self.blockSizes[x] - (tstop - bStart)
+if debug:
+print("%3d %s\t%d\t%d\t%d\t%d\t%d\t%d" %
+(x, self.strand, bStart, bEnd,
+tstart, tstop, chromStart, chromEnd), file=sys.stderr)
+bStart += self.blockSizes[x]
+return(chromStart, chromEnd)
+# get the blocks for sub range
+def get_blocks(self, chromStart, chromEnd):
+tblockCount = 0
+tblockSizes = []
+tblockStarts = []
+for x in range(self.blockCount):
+bStart = self.chromStart + self.blockStarts[x]
+bEnd = bStart + self.blockSizes[x]
+if bStart > chromEnd:
+break
+if bEnd < chromStart:
+continue
+cStart = max(chromStart, bStart)
+tblockStarts.append(cStart - chromStart)
+tblockSizes.append(min(chromEnd, bEnd) - cStart)
+tblockCount += 1
+return (tblockCount, tblockSizes, tblockStarts)
+def trim(self, tstart, tstop, debug=False):
+(tchromStart, tchromEnd) =\
+self.get_subrange(tstart, tstop, debug=debug)
+(tblockCount, tblockSizes, tblockStarts) =\
+self.get_blocks(tchromStart, tchromEnd)
+tbed = BedEntry(
+chrom=self.chrom, chromStart=tchromStart, chromEnd=tchromEnd,
+name=self.name, score=self.score, strand=self.strand,
+thickStart=tchromStart, thickEnd=tchromEnd, itemRgb=self.itemRgb,
+blockCount=tblockCount,
+blockSizes=tblockSizes, blockStarts=tblockStarts)
+if self.seq:
+ts = tchromStart-self.chromStart
+te = tchromEnd - tchromStart + ts
+tbed.seq = self.seq[ts:te]
+return tbed
+def get_filtered_translations(self, untrimmed=False, filtering=True,
+ignore_left_bp=0, ignore_right_bp=0,
+debug=False):
+translations = [None, None, None]
+seq = self.get_spliced_seq()
+ignore = (ignore_left_bp if self.strand == '+'
+else ignore_right_bp) / 3
+block_sum = sum(self.blockSizes)
+exon_sizes = [x for x in self.blockSizes]
+if self.strand == '-':
+exon_sizes.reverse()
+splice_sites = [sum(exon_sizes[:x]) / 3
+for x in range(1, len(exon_sizes))]
+if debug:
+print("splice_sites: %s" % splice_sites, file=sys.stderr)
+junc = splice_sites[0] if len(splice_sites) > 0 else exon_sizes[0]
+if seq:
+for i in range(3):
+translation = self.get_translation(sequence=seq[i:])
+if translation:
+tstart = 0
+tstop = len(translation)
+offset = (block_sum - i) % 3
+if debug:
+print("frame: %d\ttstart: %d  tstop: %d  " +
+"offset: %d\t%s" %
+(i, tstart, tstop, offset, translation),
+file=sys.stderr)
+if not untrimmed:
+tstart = translation.rfind('*', 0, junc) + 1
+stop = translation.find('*', junc)
+tstop = stop if stop >= 0 else len(translation)
+offset = (block_sum - i) % 3
+trimmed = translation[tstart:tstop]
+if debug:
+print("frame: %d\ttstart: %d  tstop: %d  " +
+"offset: %d\t%s" %
+(i, tstart, tstop, offset, trimmed),
+file=sys.stderr)
+if filtering and tstart > ignore:
+continue
+# get genomic locations for start and end
+if self.strand == '+':
+chromStart = self.chromStart + i + (tstart * 3)
+chromEnd = self.chromEnd - offset\
+- (len(translation) - tstop) * 3
+else:
+chromStart = self.chromStart + offset\
++ (len(translation) - tstop) * 3
+chromEnd = self.chromEnd - i - (tstart * 3)
+# get the blocks for this translation
+(tblockCount, tblockSizes, tblockStarts) =\
+self.get_blocks(chromStart, chromEnd)
+translations[i] = (chromStart, chromEnd, trimmed,
+tblockCount, tblockSizes, tblockStarts)
+if debug:
+print("tblockCount: %d tblockStarts: %s " +
+"tblockSizes: %s" %
+(tblockCount, tblockStarts, tblockSizes),
+file=sys.stderr)
+return translations
+def get_seq_id(self, seqtype='unk:unk', reference='', frame=None):
+# Ensembl fasta ID format
+# >ID SEQTYPE:STATUS LOCATION GENE TRANSCRIPT
+# >ENSP00000328693 pep:splice chromosome:NCBI35:1:904515:910768:1\
+#   gene:ENSG00000158815:transcript:ENST00000328693\
+#    gene_biotype:protein_coding transcript_biotype:protein_coding
+frame_name = ''
+chromStart = self.chromStart
+chromEnd = self.chromEnd
+strand = 1 if self.strand == '+' else -1
+if frame is not None:
+block_sum = sum(self.blockSizes)
+offset = (block_sum - frame) % 3
+frame_name = '_' + str(frame + 1)
+if self.strand == '+':
+chromStart += frame
+chromEnd -= offset
+else:
+chromStart += offset
+chromEnd -= frame
+location = "chromosome:%s:%s:%s:%s:%s"\
+% (reference, self.chrom, chromStart, chromEnd, strand)
+seq_id = "%s%s %s %s" % (self.name, frame_name, seqtype, location)
+return seq_id
+def get_line(self, start_offset=0, end_offset=0):
+if start_offset or end_offset:
+s_offset = start_offset if start_offset else 0
+e_offset = end_offset if end_offset else 0
+if s_offset > self.chromStart:
+s_offset = self.chromStart
+chrStart = self.chromStart - s_offset
+chrEnd = self.chromEnd + e_offset
+blkSizes = self.blockSizes
+blkSizes[0] += s_offset
+blkSizes[-1] += e_offset
+blkStarts = self.blockStarts
+for i in range(1, self.blockCount):
+blkStarts[i] += s_offset
+items = [str(x) for x in [self.chrom, chrStart, chrEnd, self.name,
+self.score, self.strand, self.thickStart,
+self.thickEnd, self.itemRgb,
+self.blockCount,
+','.join([str(x) for x in blkSizes]),
+','.join([str(x) for x in blkStarts])]]
+return '\t'.join(items) + '\n'
+return self.line

Mercurial > repos > galaxyp > retrieve_ensembl_bed

comparison bedutil.py @ 0:da1b538b87e5 draft