Functional Evaluation and Clinical Classification of BRCA2 Variants

Overview

Journal Nature

Date 2025 Jan 8

PMID 39779857

Authors

Huaizhi Huang

Chunling Hu

Jie Na

Steven N Hart

Rohan David Gnanaolivu

Mohamed Abozaid

Tara Rao

Yohannes A Tecleab

Tina Pesaran

Paulo Cilas Morais Lyra

Rachid Karam

Siddhartha Yadav

Katherine L Nathanson

Susan M Domchek

Miguel de la Hoya

Mark Robson

Miika Mehine

Chaitanya Bandlamudi

Diana Mandelker

Alvaro N A Monteiro

Edwin S Iversen

Nicholas Boddicker

Wenan Chen

Marcy E Richardson

Fergus J Couch

Affiliations

Soon will be listed here.

Abstract

Germline BRCA2 loss-of function variants, which can be identified through clinical genetic testing, predispose to several cancers. However, variants of uncertain significance limit the clinical utility of test results. Thus, there is a need for functional characterization and clinical classification of all BRCA2 variants to facilitate the clinical management of individuals with these variants. Here we analysed all possible single-nucleotide variants from exons 15 to 26 that encode the BRCA2 DNA-binding domain hotspot for pathogenic missense variants. To enable this, we used saturation genome editing CRISPR-Cas9-based knock-in endogenous targeting of human haploid HAP1 cells. The assay was calibrated relative to nonsense and silent variants and was validated using pathogenic and benign standards from ClinVar and results from a homology-directed repair functional assay. Variants (6,959 out of 6,960 evaluated) were assigned to seven categories of pathogenicity based on a VarCall Bayesian model. Single-nucleotide variants that encode loss-of-function missense variants were associated with increased risks of breast cancer and ovarian cancer. The functional assay results were integrated into models from ClinGen, the American College of Medical Genetics and Genomics, and the Association for Molecular Pathology for clinical classification of BRCA2 variants. Using this approach, 91% were classified as pathogenic or likely pathogenic or as benign or likely benign. These classified variants can be used to improve clinical management of individuals with a BRCA2 variant.

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