Actionability classification of variants of unknown significance correlates with functional effect

Author:

Johnson AmberORCID,Ng Patrick Kwok-Shing,Kahle Michael,Castillo Julia,Amador Bianca,Wang YujiaORCID,Zeng Jia,Holla Vijaykumar,Vu ThuyORCID,Su Fei,Kim Sun-Hee,Conway Tara,Jiang Xianli,Chen KenORCID,Shaw Kenna R. Mills,Yap Timothy A.ORCID,Rodon Jordi,Mills Gordon B.ORCID,Meric-Bernstam FundaORCID

Abstract

AbstractGenomically-informed therapy requires consideration of the functional impact of genomic alterations on protein expression and/or function. However, a substantial number of variants are of unknown significance (VUS). The MD Anderson Precision Oncology Decision Support (PODS) team developed an actionability classification scheme that categorizes VUS as either “Unknown” or “Potentially” actionable based on their location within functional domains and/or proximity to known oncogenic variants. We then compared PODS VUS actionability classification with results from a functional genomics platform consisting of mutant generation and cell viability assays. 106 (24%) of 438 VUS in 20 actionable genes were classified as oncogenic in functional assays. Variants categorized by PODS as Potentially actionable (N = 204) were more likely to be oncogenic than those categorized as Unknown (N = 230) (37% vs 13%, p = 4.08e-09). Our results demonstrate that rule-based actionability classification of VUS can identify patients more likely to have actionable variants for consideration with genomically-matched therapy.

Funder

Cancer Prevention and Research Institute of Texas

UTHealth | Center for Clinical and Translational Sciences, University of Texas Health Science Center at Houston

U.S. Department of Health & Human Services | NIH | National Cancer Institute

Sheikh Khalifa Bin Zayed Al Nahyan Institute for Personalized Cancer Therapy

Publisher

Springer Science and Business Media LLC

Subject

Cancer Research,Oncology

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