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""" |
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A dataset loader for the n2c2 2018 cohort selection dataset. |
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|
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The dataset consists of three archive files, |
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├── train.zip - 202 records |
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└── n2c2-t1_gold_standard_test_data.zip - 86 records |
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The individual data files (inside the zip and tar archives) come in |
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xml files that contains text as well as labels. |
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The files comprising this dataset must be on the users local machine |
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in a single directory that is passed to `datasets.load_dataset` via |
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the `data_dir` kwarg. This loader script will read the archive files |
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directly (i.e. the user should not uncompress, untar or unzip any of |
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the files). |
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Data Access from https://portal.dbmi.hms.harvard.edu/projects/n2c2-nlp/ |
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""" |
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import os |
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import zipfile |
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from collections import defaultdict |
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from typing import List |
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import datasets |
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from lxml import etree |
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from .bigbiohub import text_features |
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from .bigbiohub import BigBioConfig |
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from .bigbiohub import Tasks |
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_LANGUAGES = ['English'] |
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_PUBMED = False |
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_LOCAL = True |
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_CITATION = """\ |
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@article{DBLP:journals/jamia/StubbsFSHU19, |
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author = { |
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Amber Stubbs and |
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Michele Filannino and |
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Ergin Soysal and |
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Samuel Henry and |
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Ozlem Uzuner |
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}, |
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title = {Cohort selection for clinical trials: n2c2 2018 shared task track 1}, |
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journal = {J. Am. Medical Informatics Assoc.}, |
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volume = {26}, |
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number = {11}, |
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pages = {1163--1171}, |
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year = {2019}, |
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url = {https://doi.org/10.1093/jamia/ocz163}, |
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doi = {10.1093/jamia/ocz163}, |
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timestamp = {Mon, 15 Jun 2020 16:56:11 +0200}, |
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biburl = {https://dblp.org/rec/journals/jamia/StubbsFSHU19.bib}, |
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bibsource = {dblp computer science bibliography, https://dblp.org} |
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} |
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""" |
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_DATASETNAME = "n2c2_2018_track1" |
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_DISPLAYNAME = "n2c2 2018 Selection Criteria" |
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_DESCRIPTION = """\ |
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Track 1 of the 2018 National NLP Clinical Challenges shared tasks focused |
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on identifying which patients in a corpus of longitudinal medical records |
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meet and do not meet identified selection criteria. |
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This shared task aimed to determine whether NLP systems could be trained to identify if patients met or did not meet |
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a set of selection criteria taken from real clinical trials. The selected criteria required measurement detection ( |
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“Any HbA1c value between 6.5 and 9.5%”), inference (“Use of aspirin to prevent myocardial infarction”), |
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temporal reasoning (“Diagnosis of ketoacidosis in the past year”), and expert judgment to assess (“Major |
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diabetes-related complication”). For the corpus, we used the dataset of American English, longitudinal clinical |
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narratives from the 2014 i2b2/UTHealth shared task 4. |
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The final selected 13 selection criteria are as follows: |
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1. DRUG-ABUSE: Drug abuse, current or past |
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2. ALCOHOL-ABUSE: Current alcohol use over weekly recommended limits |
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3. ENGLISH: Patient must speak English |
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4. MAKES-DECISIONS: Patient must make their own medical decisions |
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5. ABDOMINAL: History of intra-abdominal surgery, small or large intestine |
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resection, or small bowel obstruction. |
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6. MAJOR-DIABETES: Major diabetes-related complication. For the purposes of |
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this annotation, we define “major complication” (as opposed to “minor complication”) |
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as any of the following that are a result of (or strongly correlated with) uncontrolled diabetes: |
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a. Amputation |
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b. Kidney damage |
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c. Skin conditions |
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d. Retinopathy |
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e. nephropathy |
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f. neuropathy |
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7. ADVANCED-CAD: Advanced cardiovascular disease (CAD). |
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For the purposes of this annotation, we define “advanced” as having 2 or more of the following: |
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a. Taking 2 or more medications to treat CAD |
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b. History of myocardial infarction (MI) |
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c. Currently experiencing angina |
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d. Ischemia, past or present |
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8. MI-6MOS: MI in the past 6 months |
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9. KETO-1YR: Diagnosis of ketoacidosis in the past year |
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10. DIETSUPP-2MOS: Taken a dietary supplement (excluding vitamin D) in the past 2 months |
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11. ASP-FOR-MI: Use of aspirin to prevent MI |
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12. HBA1C: Any hemoglobin A1c (HbA1c) value between 6.5% and 9.5% |
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13. CREATININE: Serum creatinine > upper limit of normal |
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The training consists of 202 patient records with document-level annotations, 10 records |
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with textual spans indicating annotator’s evidence for their annotations while test set contains 86. |
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Note: |
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* The inter-annotator average agreement is 84.9% |
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* Whereabouts of 10 records with textual spans indicating annotator’s evidence are unknown. |
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However, author did a simple script based validation to check if any of the tags contained any text |
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in any of the training set and they do not, which confirms that atleast train and test do not |
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have any evidence tagged alongside corresponding tags. |
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""" |
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_HOMEPAGE = "https://portal.dbmi.hms.harvard.edu/projects/n2c2-nlp/" |
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_LICENSE = 'Data User Agreement' |
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_SUPPORTED_TASKS = [Tasks.TEXT_CLASSIFICATION] |
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_SOURCE_VERSION = "1.0.0" |
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_BIGBIO_VERSION = "1.0.0" |
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SOURCE = "source" |
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BIGBIO_TEXT = "bigbio_text" |
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def _read_zip(file_path): |
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samples = defaultdict(dict) |
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with zipfile.ZipFile(file_path) as zf: |
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for info in zf.infolist(): |
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base, filename = os.path.split(info.filename) |
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_, ext = os.path.splitext(filename) |
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ext = ext[1:] |
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sample_id = filename.split(".")[0] |
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if ext == "xml" and not filename.startswith("."): |
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content = zf.read(info).decode("utf-8").encode() |
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root = etree.XML(content) |
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text, tags = root.getchildren() |
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samples[sample_id]["txt"] = text.text |
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samples[sample_id]["tags"] = {} |
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for child in tags: |
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samples[sample_id]["tags"][child.tag] = child.get("met") |
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return samples |
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class N2C22018CohortSelectionDataset(datasets.GeneratorBasedBuilder): |
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"""i2b2 2018 track 1 cohort selection task""" |
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SOURCE_VERSION = datasets.Version(_SOURCE_VERSION) |
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BIGBIO_VERSION = datasets.Version(_BIGBIO_VERSION) |
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_SOURCE_CONFIG_NAME = _DATASETNAME + "_" + SOURCE |
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_BIGBIO_CONFIG_NAME = _DATASETNAME + "_" + BIGBIO_TEXT |
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BUILDER_CONFIGS = [ |
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BigBioConfig( |
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name=_SOURCE_CONFIG_NAME, |
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version=SOURCE_VERSION, |
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description=_DATASETNAME + " source schema", |
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schema=SOURCE, |
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subset_id=_DATASETNAME, |
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), |
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BigBioConfig( |
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name=_BIGBIO_CONFIG_NAME, |
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version=BIGBIO_VERSION, |
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description=_DATASETNAME + " BigBio schema", |
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schema=BIGBIO_TEXT, |
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subset_id=_DATASETNAME, |
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), |
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] |
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DEFAULT_CONFIG_NAME = _SOURCE_CONFIG_NAME |
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LABEL_CLASS_NAMES = [ |
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"ABDOMINAL", |
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"ADVANCED-CAD", |
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"ALCOHOL-ABUSE", |
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"ASP-FOR-MI", |
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"CREATININE", |
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"DIETSUPP-2MOS", |
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"DRUG-ABUSE", |
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"ENGLISH", |
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"HBA1C", |
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"KETO-1YR", |
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"MAJOR-DIABETES", |
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"MAKES-DECISIONS", |
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"MI-6MOS", |
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] |
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def _info(self) -> datasets.DatasetInfo: |
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if self.config.schema == SOURCE: |
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labels = { |
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key: datasets.ClassLabel(names=["met", "not met"]) |
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for key in self.LABEL_CLASS_NAMES |
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} |
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features = datasets.Features( |
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{ |
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"id": datasets.Value("string"), |
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"document_id": datasets.Value("string"), |
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"text": datasets.Value("string"), |
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"tags": labels, |
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} |
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) |
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elif self.config.schema == BIGBIO_TEXT: |
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features = text_features |
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return datasets.DatasetInfo( |
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description=_DESCRIPTION, |
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features=features, |
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homepage=_HOMEPAGE, |
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license=str(_LICENSE), |
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citation=_CITATION, |
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) |
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def _split_generators(self, dl_manager) -> List[datasets.SplitGenerator]: |
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if self.config.data_dir is None or self.config.name is None: |
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raise ValueError( |
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"This is a local dataset. Please pass the data_dir and name kwarg to load_dataset." |
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) |
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else: |
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data_dir = self.config.data_dir |
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return [ |
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datasets.SplitGenerator( |
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name=datasets.Split.TRAIN, |
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gen_kwargs={ |
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"file_path": os.path.join(data_dir, "train.zip"), |
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}, |
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), |
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datasets.SplitGenerator( |
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name=datasets.Split.TEST, |
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gen_kwargs={ |
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"file_path": os.path.join( |
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data_dir, "n2c2-t1_gold_standard_test_data.zip" |
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), |
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}, |
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), |
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] |
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|
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@staticmethod |
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def _get_source_sample(sample_id, sample): |
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return { |
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"id": sample_id, |
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"document_id": sample_id, |
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"text": sample.get("txt", ""), |
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"tags": sample.get("tags", {}), |
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} |
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@staticmethod |
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def _get_bigbio_sample(sample_id, sample) -> dict: |
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tags = sample.get("tags", None) |
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if tags: |
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labels = [name for name, met_status in tags.items() if met_status == "met"] |
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else: |
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labels = [] |
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return { |
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"id": sample_id, |
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"document_id": sample_id, |
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"text": sample.get("txt", ""), |
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"labels": labels, |
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} |
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|
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def _generate_examples(self, file_path): |
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samples = _read_zip(file_path) |
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_id = 0 |
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for sample_id, sample in samples.items(): |
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if self.config.name == self._SOURCE_CONFIG_NAME: |
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yield _id, self._get_source_sample(sample_id, sample) |
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elif self.config.name == self._BIGBIO_CONFIG_NAME: |
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yield _id, self._get_bigbio_sample(sample_id, sample) |
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_id += 1 |
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