Phenotype Risk Scores Identify Patients with Unrecognized Mendelian Disease Patterns

Overview

Journal Science

Specialty Science

Date 2018 Mar 29

PMID 29590070

Citations 103

Authors

Lisa Bastarache

Jacob J Hughey

Scott Hebbring

Joy Marlo

Wanke Zhao

Wanting T Ho

Sara L Van Driest

Tracy L McGregor

Jonathan D Mosley

Quinn S Wells

Michael Temple

Andrea H Ramirez

Robert Carroll

Travis Osterman

Todd Edwards

Douglas Ruderfer

Digna R Velez Edwards

Rizwan Hamid

Joy Cogan

Andrew Glazer

Wei-Qi Wei

Qiping Feng

Murray Brilliant

Zhizhuang J Zhao

Nancy J Cox

Dan M Roden

Joshua C Denny

Affiliations

Soon will be listed here.

Abstract

Genetic association studies often examine features independently, potentially missing subpopulations with multiple phenotypes that share a single cause. We describe an approach that aggregates phenotypes on the basis of patterns described by Mendelian diseases. We mapped the clinical features of 1204 Mendelian diseases into phenotypes captured from the electronic health record (EHR) and summarized this evidence as phenotype risk scores (PheRSs). In an initial validation, PheRS distinguished cases and controls of five Mendelian diseases. Applying PheRS to 21,701 genotyped individuals uncovered 18 associations between rare variants and phenotypes consistent with Mendelian diseases. In 16 patients, the rare genetic variants were associated with severe outcomes such as organ transplants. PheRS can augment rare-variant interpretation and may identify subsets of patients with distinct genetic causes for common diseases.

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