Actionable exomic incidental findings in 6503 participants: challenges of variant classification

Author:

Amendola Laura M.,Dorschner Michael O.,Robertson Peggy D.,Salama Joseph S.,Hart Ragan,Shirts Brian H.,Murray Mitzi L.,Tokita Mari J.,Gallego Carlos J.,Kim Daniel Seung,Bennett James T.,Crosslin David R.,Ranchalis Jane,Jones Kelly L.,Rosenthal Elisabeth A.,Jarvik Ella R.,Itsara Andy,Turner Emily H.,Herman Daniel S.,Schleit Jennifer,Burt Amber,Jamal Seema M.,Abrudan Jenica L.,Johnson Andrew D.,Conlin Laura K.,Dulik Matthew C.,Santani Avni,Metterville Danielle R.,Kelly Melissa,Foreman Ann Katherine M.,Lee Kristy,Taylor Kent D.,Guo Xiuqing,Crooks Kristy,Kiedrowski Lesli A.,Raffel Leslie J.,Gordon Ora,Machini Kalotina,Desnick Robert J.,Biesecker Leslie G.,Lubitz Steven A.,Mulchandani Surabhi,Cooper Greg M.,Joffe Steven,Richards C. Sue,Yang Yaoping,Rotter Jerome I.,Rich Stephen S.,O’Donnell Christopher J.,Berg Jonathan S.,Spinner Nancy B.,Evans James P.,Fullerton Stephanie M.,Leppig Kathleen A.,Bennett Robin L.,Bird Thomas,Sybert Virginia P.,Grady William M.,Tabor Holly K.,Kim Jerry H.,Bamshad Michael J.,Wilfond Benjamin,Motulsky Arno G.,Scott C. Ronald,Pritchard Colin C.,Walsh Tom D.,Burke Wylie,Raskind Wendy H.,Byers Peter,Hisama Fuki M.,Rehm Heidi,Nickerson Debbie A.,Jarvik Gail P.

Abstract

Recommendations for laboratories to report incidental findings from genomic tests have stimulated interest in such results. In order to investigate the criteria and processes for assigning the pathogenicity of specific variants and to estimate the frequency of such incidental findings in patients of European and African ancestry, we classified potentially actionable pathogenic single-nucleotide variants (SNVs) in all 4300 European- and 2203 African-ancestry participants sequenced by the NHLBI Exome Sequencing Project (ESP). We considered 112 gene-disease pairs selected by an expert panel as associated with medically actionable genetic disorders that may be undiagnosed in adults. The resulting classifications were compared to classifications from other clinical and research genetic testing laboratories, as well as with in silico pathogenicity scores. Among European-ancestry participants, 30 of 4300 (0.7%) had a pathogenic SNV and six (0.1%) had a disruptive variant that was expected to be pathogenic, whereas 52 (1.2%) had likely pathogenic SNVs. For African-ancestry participants, six of 2203 (0.3%) had a pathogenic SNV and six (0.3%) had an expected pathogenic disruptive variant, whereas 13 (0.6%) had likely pathogenic SNVs. Genomic Evolutionary Rate Profiling mammalian conservation score and the Combined Annotation Dependent Depletion summary score of conservation, substitution, regulation, and other evidence were compared across pathogenicity assignments and appear to have utility in variant classification. This work provides a refined estimate of the burden of adult onset, medically actionable incidental findings expected from exome sequencing, highlights challenges in variant classification, and demonstrates the need for a better curated variant interpretation knowledge base.

Funder

NIH, NHGRI/NCI

NIH/NIGMS

Washington State Life Sciences Discovery Fund

NHLBI

Publisher

Cold Spring Harbor Laboratory

Subject

Genetics(clinical),Genetics

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