Functional Analysis of Clinical Germline Variants

Overview

Journal Cold Spring Harb Mol Case Stud

Specialty Genetics

Date 2019 Aug 3

PMID 31371347

Citations 3

Authors

Ming Ren Toh

Siao Ting Chong

Sock Hoai Chan

Chen Ee Low

Nur Diana Binte Ishak

Jing Quan Lim

Eliza Courtney

Joanne Ngeow

Affiliations

Soon will be listed here.

Abstract

Germline pathogenic variants in account for one-third of familial breast cancers. The majority of function requires heterodimerization with In contrast to , is a low-penetrance gene with an unclear clinical relevance, partly because of limited functional evidence. Using patient-derived lymphoblastoid cells, we functionally characterized two pathogenic variants (c.1833dupT, c.2099delG) and three variants of uncertain significance (VUSs) (c.73G>C, c.1217G>A, c.1918C>A). Three of these patients had breast cancers, whereas the remaining had colorectal cancers ( = 3). Both patients with pathogenic variants (c.1833dupT, c.2099delG) developed breast cancers with aggressive disease phenotypes such as triple-negative breast cancer and high cancer grades. As encompasses multiple functional domains, including those of apoptosis and homologous recombination repair, we hypothesized that the function being impaired would correspond with the domain where the variant was located. Variants c.1918C>A, c.1833dupT, c.1217G>A, and c.2099delG, located within and proximal to apoptotic domains of ankyrin and BRCT, were associated with impaired apoptosis. Conversely, apoptosis function was preserved in c.73G>C, which was distant from the ankyrin domain. All variants displayed normal BRCA1 heterodimerization and RAD51 colocalization, consistent with their location being distal to BRCA1-and RAD51-binding domains. In view of deficient apoptosis, VUSs (c.1217G>A and c.1918C>A) may be pathogenic or likely pathogenic variants. In summary, functional analysis of VUSs requires a combination of assays and, more importantly, the use of appropriate functional assays with consideration to the variant's location.

Citing Articles

Germline heterozygous exons 8-11 pathogenic BARD1 gene deletion reported for the first time in a family with suspicion of a hereditary colorectal cancer syndrome: more than an incidental finding?.

Carrera S, Rodriguez-Martinez A, Garin I, Sarasola E, Martinez C, Maortua H Hered Cancer Clin Pract. 2023; 21(1):2.

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Literature Review of as a Cancer Predisposing Gene with a Focus on Breast and Ovarian Cancers.

Alenezi W, Fierheller C, Recio N, Tonin P Genes (Basel). 2020; 11(8).

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The Effects of Genetic and Epigenetic Alterations of BARD1 on the Development of Non-Breast and Non-Gynecological Cancers.

Watters A, Seltzer E, MacKenzie Jr D, Young M, Muratori J, Hussein R Genes (Basel). 2020; 11(7).

PMID: 32708251 PMC: 7396976. DOI: 10.3390/genes11070829.

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