Linking glycemic dysregulation in diabetes to symptoms, comorbidities, and genetics through EHR data mining

Diabetes is a diverse and complex disease, with considerable variation in phenotypic manifestation and severity. This variation hampers the study of etiological differences and reduces the statistical power of analyses of associations to genetics, treatment outcomes, and complications. We address th...

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Published ineLife Vol. 8
Main Authors Kirk, Isa Kristina, Simon, Christian, Banasik, Karina, Holm, Peter Christoffer, Haue, Amalie Dahl, Jensen, Peter Bjødstrup, Juhl Jensen, Lars, Rodríguez, Cristina Leal, Pedersen, Mette Krogh, Eriksson, Robert, Andersen, Henrik Ullits, Almdal, Thomas, Bork-Jensen, Jette, Grarup, Niels, Borch-Johnsen, Knut, Pedersen, Oluf, Pociot, Flemming, Hansen, Torben, Bergholdt, Regine, Rossing, Peter, Brunak, Søren
Format Journal Article
LanguageEnglish
Published England eLife Sciences Publications Ltd 10.12.2019
eLife Sciences Publications, Ltd
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Summary:Diabetes is a diverse and complex disease, with considerable variation in phenotypic manifestation and severity. This variation hampers the study of etiological differences and reduces the statistical power of analyses of associations to genetics, treatment outcomes, and complications. We address these issues through deep, fine-grained phenotypic stratification of a diabetes cohort. Text mining the electronic health records of 14,017 patients, we matched two controlled vocabularies (ICD-10 and a custom vocabulary developed at the clinical center Steno Diabetes Center Copenhagen) to clinical narratives spanning a 19 year period. The two matched vocabularies comprise over 20,000 medical terms describing symptoms, other diagnoses, and lifestyle factors. The cohort is genetically homogeneous (Caucasian diabetes patients from Denmark) so the resulting stratification is not driven by ethnic differences, but rather by inherently dissimilar progression patterns and lifestyle related risk factors. Using unsupervised Markov clustering, we defined 71 clusters of at least 50 individuals within the diabetes spectrum. The clusters display both distinct and shared longitudinal glycemic dysregulation patterns, temporal co-occurrences of comorbidities, and associations to single nucleotide polymorphisms in or near genes relevant for diabetes comorbidities.
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These authors contributed equally to this work.
ISSN:2050-084X
2050-084X
DOI:10.7554/eLife.44941