# Copyright 2010 by Andrea Pierleoni # Revisions copyright 2010 by Peter Cock # All rights reserved. # # This code is part of the Biopython distribution and governed by its # license. Please see the LICENSE file that should have been included # as part of this package. """Bio.SeqIO support for the "uniprot-xml" file format. See also: http://www.uniprot.org The UniProt XML format essentially replaces the old plain text file format originally introduced by SwissProt ("swiss" format in Bio.SeqIO). """ import sys from Bio import Seq from Bio import SeqFeature from Bio import Alphabet from Bio.SeqRecord import SeqRecord from Bio._py3k import StringIO #For speed try to use cElementTree rather than ElementTree try: if (3, 0) <= sys.version_info[:2] <= (3, 1): # Workaround for bug in python 3.0 and 3.1, # see http://bugs.python.org/issue9257 from xml.etree import ElementTree as ElementTree else: from xml.etree import cElementTree as ElementTree except ImportError: from xml.etree import ElementTree as ElementTree NS = "{http://uniprot.org/uniprot}" REFERENCE_JOURNAL = "%(name)s %(volume)s:%(first)s-%(last)s(%(pub_date)s)" def UniprotIterator(handle, alphabet=Alphabet.ProteinAlphabet(), return_raw_comments=False): """Generator function to parse UniProt XML as SeqRecord objects. parses an XML entry at a time from any UniProt XML file returns a SeqRecord for each iteration This generator can be used in Bio.SeqIO return_raw_comments = True --> comment fields are returned as complete XML to allow further processing skip_parsing_errors = True --> if parsing errors are found, skip to next entry """ if isinstance(alphabet, Alphabet.NucleotideAlphabet): raise ValueError("Wrong alphabet %r" % alphabet) if isinstance(alphabet, Alphabet.Gapped): if isinstance(alphabet.alphabet, Alphabet.NucleotideAlphabet): raise ValueError("Wrong alphabet %r" % alphabet) if not hasattr(handle, "read"): if isinstance(handle, str): handle = StringIO(handle) else: raise Exception('An XML-containing handler or an XML string must be passed') if ElementTree is None: from Bio import MissingExternalDependencyError raise MissingExternalDependencyError( "No ElementTree module was found. " "Use Python 2.5+, lxml or elementtree if you " "want to use Bio.SeqIO.UniprotIO.") for event, elem in ElementTree.iterparse(handle, events=("start", "end")): if event == "end" and elem.tag == NS + "entry": yield Parser(elem, alphabet=alphabet, return_raw_comments=return_raw_comments).parse() elem.clear() class Parser(object): """Parse a UniProt XML entry to a SeqRecord. return_raw_comments=True to get back the complete comment field in XML format alphabet=Alphabet.ProteinAlphabet() can be modified if needed, default is protein alphabet. """ def __init__(self, elem, alphabet=Alphabet.ProteinAlphabet(), return_raw_comments=False): self.entry = elem self.alphabet = alphabet self.return_raw_comments = return_raw_comments def parse(self): """Parse the input.""" assert self.entry.tag == NS + 'entry' def append_to_annotations(key, value): if key not in self.ParsedSeqRecord.annotations: self.ParsedSeqRecord.annotations[key] = [] if value not in self.ParsedSeqRecord.annotations[key]: self.ParsedSeqRecord.annotations[key].append(value) def _parse_name(element): self.ParsedSeqRecord.name = element.text self.ParsedSeqRecord.dbxrefs.append(self.dbname + ':' + element.text) def _parse_accession(element): append_to_annotations('accessions', element.text) # to cope with SwissProt plain text parser self.ParsedSeqRecord.dbxrefs.append(self.dbname + ':' + element.text) def _parse_protein(element): """Parse protein names (PRIVATE).""" descr_set = False for protein_element in element: if protein_element.tag in [NS + 'recommendedName', NS + 'alternativeName']: # recommendedName tag are parsed before #use protein fields for name and description for rec_name in protein_element: ann_key = '%s_%s' % (protein_element.tag.replace(NS, ''), rec_name.tag.replace(NS, '')) append_to_annotations(ann_key, rec_name.text) if (rec_name.tag == NS + 'fullName') and not descr_set: self.ParsedSeqRecord.description = rec_name.text descr_set = True elif protein_element.tag == NS + 'component': pass # not parsed elif protein_element.tag == NS + 'domain': pass # not parsed def _parse_gene(element): for genename_element in element: if 'type' in genename_element.attrib: ann_key = 'gene_%s_%s' % (genename_element.tag.replace(NS, ''), genename_element.attrib['type']) if genename_element.attrib['type'] == 'primary': self.ParsedSeqRecord.annotations[ann_key] = genename_element.text else: append_to_annotations(ann_key, genename_element.text) def _parse_geneLocation(element): append_to_annotations('geneLocation', element.attrib['type']) def _parse_organism(element): organism_name = com_name = sci_name = '' for organism_element in element: if organism_element.tag == NS + 'name': if organism_element.text: if organism_element.attrib['type'] == 'scientific': sci_name = organism_element.text elif organism_element.attrib['type'] == 'common': com_name = organism_element.text else: #e.g. synonym append_to_annotations("organism_name", organism_element.text) elif organism_element.tag == NS + 'dbReference': self.ParsedSeqRecord.dbxrefs.append(organism_element.attrib['type'] + ':' + organism_element.attrib['id']) elif organism_element.tag == NS + 'lineage': for taxon_element in organism_element: if taxon_element.tag == NS + 'taxon': append_to_annotations('taxonomy', taxon_element.text) if sci_name and com_name: organism_name = '%s (%s)' % (sci_name, com_name) elif sci_name: organism_name = sci_name elif com_name: organism_name = com_name self.ParsedSeqRecord.annotations['organism'] = organism_name def _parse_organismHost(element): for organism_element in element: if organism_element.tag == NS + 'name': append_to_annotations("organism_host", organism_element.text) def _parse_keyword(element): append_to_annotations('keywords', element.text) def _parse_comment(element): """Parse comments (PRIVATE). Comment fields are very heterogeneus. each type has his own (frequently mutated) schema. To store all the contained data, more complex data structures are needed, such as annotated dictionaries. This is left to end user, by optionally setting: return_raw_comments=True The original XML is returned in the annotation fields. Available comment types at december 2009: "allergen" "alternative products" "biotechnology" "biophysicochemical properties" "catalytic activity" "caution" "cofactor" "developmental stage" "disease" "domain" "disruption phenotype" "enzyme regulation" "function" "induction" "miscellaneous" "pathway" "pharmaceutical" "polymorphism" "PTM" "RNA editing" "similarity" "subcellular location" "sequence caution" "subunit" "tissue specificity" "toxic dose" "online information" "mass spectrometry" "interaction" """ simple_comments = ["allergen", "biotechnology", "biophysicochemical properties", "catalytic activity", "caution", "cofactor", "developmental stage", "disease", "domain", "disruption phenotype", "enzyme regulation", "function", "induction", "miscellaneous", "pathway", "pharmaceutical", "polymorphism", "PTM", "RNA editing", # positions not parsed "similarity", "subunit", "tissue specificity", "toxic dose", ] if element.attrib['type'] in simple_comments: ann_key = 'comment_%s' % element.attrib['type'].replace(' ', '') for text_element in element.getiterator(NS + 'text'): if text_element.text: append_to_annotations(ann_key, text_element.text) elif element.attrib['type'] == 'subcellular location': for subloc_element in element.getiterator(NS + 'subcellularLocation'): for el in subloc_element: if el.text: ann_key = 'comment_%s_%s' % (element.attrib['type'].replace(' ', ''), el.tag.replace(NS, '')) append_to_annotations(ann_key, el.text) elif element.attrib['type'] == 'interaction': for interact_element in element.getiterator(NS + 'interactant'): ann_key = 'comment_%s_intactId' % element.attrib['type'] append_to_annotations(ann_key, interact_element.attrib['intactId']) elif element.attrib['type'] == 'alternative products': for alt_element in element.getiterator(NS + 'isoform'): ann_key = 'comment_%s_isoform' % element.attrib['type'].replace(' ', '') for id_element in alt_element.getiterator(NS + 'id'): append_to_annotations(ann_key, id_element.text) elif element.attrib['type'] == 'mass spectrometry': ann_key = 'comment_%s' % element.attrib['type'].replace(' ', '') start = end = 0 for loc_element in element.getiterator(NS + 'location'): pos_els = loc_element.getiterator(NS + 'position') pos_els = list(pos_els) # this try should be avoided, maybe it is safer to skip position parsing for mass spectrometry try: if pos_els: end = int(pos_els[0].attrib['position']) start = end - 1 else: start = int(list(loc_element.getiterator(NS + 'begin'))[0].attrib['position']) - 1 end = int(list(loc_element.getiterator(NS + 'end'))[0].attrib['position']) except: # undefined positions or erroneously mapped pass mass = element.attrib['mass'] method = element.attrib['method'] if start == end == 0: append_to_annotations(ann_key, 'undefined:%s|%s' % (mass, method)) else: append_to_annotations(ann_key, '%s..%s:%s|%s' % (start, end, mass, method)) elif element.attrib['type'] == 'sequence caution': pass # not parsed: few information, complex structure elif element.attrib['type'] == 'online information': for link_element in element.getiterator(NS + 'link'): ann_key = 'comment_%s' % element.attrib['type'].replace(' ', '') for id_element in link_element.getiterator(NS + 'link'): append_to_annotations(ann_key, '%s@%s' % (element.attrib['name'], link_element.attrib['uri'])) #return raw XML comments if needed if self.return_raw_comments: ann_key = 'comment_%s_xml' % element.attrib['type'].replace(' ', '') append_to_annotations(ann_key, ElementTree.tostring(element)) def _parse_dbReference(element): self.ParsedSeqRecord.dbxrefs.append(element.attrib['type'] + ':' + element.attrib['id']) #e.g. # # # # # if 'type' in element.attrib: if element.attrib['type'] == 'PDB': method = "" resolution = "" for ref_element in element: if ref_element.tag == NS + 'property': dat_type = ref_element.attrib['type'] if dat_type == 'method': method = ref_element.attrib['value'] if dat_type == 'resolution': resolution = ref_element.attrib['value'] if dat_type == 'chains': pairs = ref_element.attrib['value'].split(',') for elem in pairs: pair = elem.strip().split('=') if pair[1] != '-': #TODO - How best to store these, do SeqFeatures make sense? feature = SeqFeature.SeqFeature() feature.type = element.attrib['type'] feature.qualifiers['name'] = element.attrib['id'] feature.qualifiers['method'] = method feature.qualifiers['resolution'] = resolution feature.qualifiers['chains'] = pair[0].split('/') start = int(pair[1].split('-')[0]) - 1 end = int(pair[1].split('-')[1]) feature.location = SeqFeature.FeatureLocation(start, end) #self.ParsedSeqRecord.features.append(feature) for ref_element in element: if ref_element.tag == NS + 'property': pass # this data cannot be fitted in a seqrecord object with a simple list. however at least ensembl and EMBL parsing can be improved to add entries in dbxrefs def _parse_reference(element): reference = SeqFeature.Reference() authors = [] scopes = [] tissues = [] journal_name = '' pub_type = '' pub_date = '' for ref_element in element: if ref_element.tag == NS + 'citation': pub_type = ref_element.attrib['type'] if pub_type == 'submission': pub_type += ' to the ' + ref_element.attrib['db'] if 'name' in ref_element.attrib: journal_name = ref_element.attrib['name'] pub_date = ref_element.attrib.get('date', '') j_volume = ref_element.attrib.get('volume', '') j_first = ref_element.attrib.get('first', '') j_last = ref_element.attrib.get('last', '') for cit_element in ref_element: if cit_element.tag == NS + 'title': reference.title = cit_element.text elif cit_element.tag == NS + 'authorList': for person_element in cit_element: authors.append(person_element.attrib['name']) elif cit_element.tag == NS + 'dbReference': self.ParsedSeqRecord.dbxrefs.append(cit_element.attrib['type'] + ':' + cit_element.attrib['id']) if cit_element.attrib['type'] == 'PubMed': reference.pubmed_id = cit_element.attrib['id'] elif ref_element.attrib['type'] == 'MEDLINE': reference.medline_id = cit_element.attrib['id'] elif ref_element.tag == NS + 'scope': scopes.append(ref_element.text) elif ref_element.tag == NS + 'source': for source_element in ref_element: if source_element.tag == NS + 'tissue': tissues.append(source_element.text) if scopes: scopes_str = 'Scope: ' + ', '.join(scopes) else: scopes_str = '' if tissues: tissues_str = 'Tissue: ' + ', '.join(tissues) else: tissues_str = '' # locations cannot be parsed since they are actually written in # free text inside scopes so all the references are put in the # annotation. reference.location = [] reference.authors = ', '.join(authors) if journal_name: if pub_date and j_volume and j_first and j_last: reference.journal = REFERENCE_JOURNAL % dict(name=journal_name, volume=j_volume, first=j_first, last=j_last, pub_date=pub_date) else: reference.journal = journal_name reference.comment = ' | '.join((pub_type, pub_date, scopes_str, tissues_str)) append_to_annotations('references', reference) def _parse_position(element, offset=0): try: position = int(element.attrib['position']) + offset except KeyError as err: position = None status = element.attrib.get('status', '') if status == 'unknown': assert position is None return SeqFeature.UnknownPosition() elif not status: return SeqFeature.ExactPosition(position) elif status == 'greater than': return SeqFeature.AfterPosition(position) elif status == 'less than': return SeqFeature.BeforePosition(position) elif status == 'uncertain': return SeqFeature.UncertainPosition(position) else: raise NotImplementedError("Position status %r" % status) def _parse_feature(element): feature = SeqFeature.SeqFeature() for k, v in element.attrib.items(): feature.qualifiers[k] = v feature.type = element.attrib.get('type', '') if 'id' in element.attrib: feature.id = element.attrib['id'] for feature_element in element: if feature_element.tag == NS + 'location': position_elements = feature_element.findall(NS + 'position') if position_elements: element = position_elements[0] start_position = _parse_position(element, -1) end_position = _parse_position(element) else: element = feature_element.findall(NS + 'begin')[0] start_position = _parse_position(element, -1) element = feature_element.findall(NS + 'end')[0] end_position = _parse_position(element) feature.location = SeqFeature.FeatureLocation(start_position, end_position) else: try: feature.qualifiers[feature_element.tag.replace(NS, '')] = feature_element.text except: pass # skip unparsable tag self.ParsedSeqRecord.features.append(feature) def _parse_proteinExistence(element): append_to_annotations('proteinExistence', element.attrib['type']) def _parse_evidence(element): for k, v in element.attrib.items(): ann_key = k append_to_annotations(ann_key, v) def _parse_sequence(element): for k, v in element.attrib.items(): if k in ("length", "mass", "version"): self.ParsedSeqRecord.annotations['sequence_%s' % k] = int(v) else: self.ParsedSeqRecord.annotations['sequence_%s' % k] = v seq = ''.join((element.text.split())) self.ParsedSeqRecord.seq = Seq.Seq(seq, self.alphabet) #============================================# #Initialize SeqRecord self.ParsedSeqRecord = SeqRecord('', id='') #Entry attribs parsing #Unknown dataset should not happen! self.dbname = self.entry.attrib.get('dataset', 'UnknownDataset') #add attribs to annotations for k, v in self.entry.attrib.items(): if k in ("version"): #original #self.ParsedSeqRecord.annotations["entry_%s" % k] = int(v) #To cope with swissProt plain text parser. this can cause errors #if the attrib has the same name of an other annotation self.ParsedSeqRecord.annotations[k] = int(v) else: #self.ParsedSeqRecord.annotations["entry_%s" % k] = v self.ParsedSeqRecord.annotations[k] = v # to cope with swissProt plain text parser #Top-to-bottom entry children parsing for element in self.entry: if element.tag == NS + 'name': _parse_name(element) elif element.tag == NS + 'accession': _parse_accession(element) elif element.tag == NS + 'protein': _parse_protein(element) elif element.tag == NS + 'gene': _parse_gene(element) elif element.tag == NS + 'geneLocation': _parse_geneLocation(element) elif element.tag == NS + 'organism': _parse_organism(element) elif element.tag == NS + 'organismHost': _parse_organismHost(element) elif element.tag == NS + 'keyword': _parse_keyword(element) elif element.tag == NS + 'comment': _parse_comment(element) elif element.tag == NS + 'dbReference': _parse_dbReference(element) elif element.tag == NS + 'reference': _parse_reference(element) elif element.tag == NS + 'feature': _parse_feature(element) elif element.tag == NS + 'proteinExistence': _parse_proteinExistence(element) elif element.tag == NS + 'evidence': _parse_evidence(element) elif element.tag == NS + 'sequence': _parse_sequence(element) else: pass #remove duplicate dbxrefs self.ParsedSeqRecord.dbxrefs = sorted(list(set(self.ParsedSeqRecord.dbxrefs))) # use first accession as id if not self.ParsedSeqRecord.id: self.ParsedSeqRecord.id = self.ParsedSeqRecord.annotations['accessions'][0] return self.ParsedSeqRecord