Value of the loss of heterozygosity to BRCA1 variant classification

Author:

Santana dos Santos ElizabethORCID,Spurdle Amanda B.ORCID,Carraro Dirce M.,Briaux Adrien,Southey MelissaORCID,Torrezan GiovanaORCID,Petitalot Ambre,Leman Raphael,Lafitte Philippe,Meseure Didier,Driouch Keltouma,Side Lucy,Brewer Carole,Beck Sarah,Melville Athalie,Callaway Alison,Revillion Françoise,Folgueira Maria A. A. Koike,Parsons Michael T.ORCID,Thorne Heather,Vincent-Salomon AnneORCID,Stoppa-Lyonnet Dominique,Bieche Ivan,Caputo Sandrine M.,Rouleau Etienne,

Abstract

AbstractAt least 10% of the BRCA1/2 tests identify variants of uncertain significance (VUS) while the distinction between pathogenic variants (PV) and benign variants (BV) remains particularly challenging. As a typical tumor suppressor gene, the inactivation of the second wild-type (WT) BRCA1 allele is expected to trigger cancer initiation. Loss of heterozygosity (LOH) of the WT allele is the most frequent mechanism for the BRCA1 biallelic inactivation. To evaluate if LOH can be an effective predictor of BRCA1 variant pathogenicity, we carried out LOH analysis on DNA extracted from 90 breast and seven ovary tumors diagnosed in 27 benign and 55 pathogenic variant carriers. Further analyses were conducted in tumors with PVs yet without loss of the WT allele: BRCA1 promoter hypermethylation, next-generation sequencing (NGS) of BRCA1/2, and BRCAness score. Ninety-seven tumor samples were analyzed from 26 different BRCA1 variants. A relatively stable pattern of LOH (65.4%) of WT allele for PV tumors was observed, while the allelic balance (63%) or loss of variant allele (15%) was generally seen for carriers of BV. LOH data is a useful complementary argument for BRCA1 variant classification.

Publisher

Springer Science and Business Media LLC

Subject

Pharmacology (medical),Radiology, Nuclear Medicine and imaging,Oncology

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