Evaluating the Clinical Validity of Gene-Disease Associations: An Evidence-Based Framework Developed by the Clinical Genome Resource

Overview

Journal Am J Hum Genet

Publisher Cell Press

Specialty Genetics

Date 2017 May 30

PMID 28552198

Citations 264

Authors

Natasha T Strande

Erin Rooney Riggs

Adam H Buchanan

Ozge Ceyhan-Birsoy

Marina DiStefano

Selina S Dwight

Jenny Goldstein

Rajarshi Ghosh

Bryce A Seifert

Tam P Sneddon

Matt W Wright

Laura V Milko

J Michael Cherry

Monica A Giovanni

Michael F Murray

Julianne M ODaniel

Erin M Ramos

Avni B Santani

Alan F Scott

Sharon E Plon

Heidi L Rehm

Christa L Martin

Jonathan S Berg

Affiliations

Soon will be listed here.

Abstract

With advances in genomic sequencing technology, the number of reported gene-disease relationships has rapidly expanded. However, the evidence supporting these claims varies widely, confounding accurate evaluation of genomic variation in a clinical setting. Despite the critical need to differentiate clinically valid relationships from less well-substantiated relationships, standard guidelines for such evaluation do not currently exist. The NIH-funded Clinical Genome Resource (ClinGen) has developed a framework to define and evaluate the clinical validity of gene-disease pairs across a variety of Mendelian disorders. In this manuscript we describe a proposed framework to evaluate relevant genetic and experimental evidence supporting or contradicting a gene-disease relationship and the subsequent validation of this framework using a set of representative gene-disease pairs. The framework provides a semiquantitative measurement for the strength of evidence of a gene-disease relationship that correlates to a qualitative classification: "Definitive," "Strong," "Moderate," "Limited," "No Reported Evidence," or "Conflicting Evidence." Within the ClinGen structure, classifications derived with this framework are reviewed and confirmed or adjusted based on clinical expertise of appropriate disease experts. Detailed guidance for utilizing this framework and access to the curation interface is available on our website. This evidence-based, systematic method to assess the strength of gene-disease relationships will facilitate more knowledgeable utilization of genomic variants in clinical and research settings.

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