Functional analysis of BARD1 missense variants in homology-directed repair and damage sensitivity.

Functional analysis of BARD1 missense variants in homology-directed repair and damage sensitivity.

The BARD1 protein, which heterodimerizes with BRCA1, is encoded by a known breast cancer susceptibility gene. While several BARD1 variants have been identified as pathogenic, many more missense variants exist that do not occur frequently enough to assign a clinical risk. In this paper, whole exome s...

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Main Authors: Aleksandra I Adamovich, Tapahsama Banerjee, Margaret Wingo, Kathryn Duncan, Jie Ning, Fernanda Martins Rodrigues, Kuan-Lin Huang, Cindy Lee, Feng Chen, Li Ding, Jeffrey D Parvin
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2019-03-01
Series:PLoS Genetics
Online Access:http://europepmc.org/articles/PMC6457558?pdf=render
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spelling doaj-5a71d84b94f7450ca925ff8d645142202020-11-24T22:06:48ZengPublic Library of Science (PLoS)PLoS Genetics1553-73901553-74042019-03-01153e100804910.1371/journal.pgen.1008049Functional analysis of BARD1 missense variants in homology-directed repair and damage sensitivity.Aleksandra I AdamovichTapahsama BanerjeeMargaret WingoKathryn DuncanJie NingFernanda Martins RodriguesKuan-Lin HuangCindy LeeFeng ChenLi DingJeffrey D ParvinThe BARD1 protein, which heterodimerizes with BRCA1, is encoded by a known breast cancer susceptibility gene. While several BARD1 variants have been identified as pathogenic, many more missense variants exist that do not occur frequently enough to assign a clinical risk. In this paper, whole exome sequencing of over 10,000 cancer samples from 33 cancer types identified from somatic mutations and loss of heterozygosity in tumors 76 potentially cancer-associated BARD1 missense and truncation variants. These variants were tested in a functional assay for homology-directed repair (HDR), as HDR deficiencies have been shown to correlate with clinical pathogenicity for BRCA1 variants. From these 76 variants, 4 in the ankyrin repeat domain and 5 in the BRCT domain were found to be non-functional in HDR. Two known benign variants were found to be functional in HDR, and three known pathogenic variants were non-functional, supporting the notion that the HDR assay can be used to predict the clinical risk of BARD1 variants. The identification of HDR-deficient variants in the ankyrin repeat domain indicates there are DNA repair functions associated with this domain that have not been closely examined. In order to examine whether BARD1-associated loss of HDR function results in DNA damage sensitivity, cells expressing non-functional BARD1 variants were treated with ionizing radiation or cisplatin. These cells were found to be more sensitive to DNA damage, and variations in the residual HDR function of non-functional variants did not correlate with variations in sensitivity. These findings improve the understanding of BARD1 functional domains in DNA repair and support that this functional assay is useful for predicting the cancer association of BARD1 variants.http://europepmc.org/articles/PMC6457558?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Aleksandra I Adamovich
Tapahsama Banerjee
Margaret Wingo
Kathryn Duncan
Jie Ning
Fernanda Martins Rodrigues
Kuan-Lin Huang
Cindy Lee
Feng Chen
Li Ding
Jeffrey D Parvin
spellingShingle Aleksandra I Adamovich
Tapahsama Banerjee
Margaret Wingo
Kathryn Duncan
Jie Ning
Fernanda Martins Rodrigues
Kuan-Lin Huang
Cindy Lee
Feng Chen
Li Ding
Jeffrey D Parvin
Functional analysis of BARD1 missense variants in homology-directed repair and damage sensitivity.
PLoS Genetics
author_facet Aleksandra I Adamovich
Tapahsama Banerjee
Margaret Wingo
Kathryn Duncan
Jie Ning
Fernanda Martins Rodrigues
Kuan-Lin Huang
Cindy Lee
Feng Chen
Li Ding
Jeffrey D Parvin
author_sort Aleksandra I Adamovich
title Functional analysis of BARD1 missense variants in homology-directed repair and damage sensitivity.
title_short Functional analysis of BARD1 missense variants in homology-directed repair and damage sensitivity.
title_full Functional analysis of BARD1 missense variants in homology-directed repair and damage sensitivity.
title_fullStr Functional analysis of BARD1 missense variants in homology-directed repair and damage sensitivity.
title_full_unstemmed Functional analysis of BARD1 missense variants in homology-directed repair and damage sensitivity.
title_sort functional analysis of bard1 missense variants in homology-directed repair and damage sensitivity.
publisher Public Library of Science (PLoS)
series PLoS Genetics
issn 1553-7390
1553-7404
publishDate 2019-03-01
description The BARD1 protein, which heterodimerizes with BRCA1, is encoded by a known breast cancer susceptibility gene. While several BARD1 variants have been identified as pathogenic, many more missense variants exist that do not occur frequently enough to assign a clinical risk. In this paper, whole exome sequencing of over 10,000 cancer samples from 33 cancer types identified from somatic mutations and loss of heterozygosity in tumors 76 potentially cancer-associated BARD1 missense and truncation variants. These variants were tested in a functional assay for homology-directed repair (HDR), as HDR deficiencies have been shown to correlate with clinical pathogenicity for BRCA1 variants. From these 76 variants, 4 in the ankyrin repeat domain and 5 in the BRCT domain were found to be non-functional in HDR. Two known benign variants were found to be functional in HDR, and three known pathogenic variants were non-functional, supporting the notion that the HDR assay can be used to predict the clinical risk of BARD1 variants. The identification of HDR-deficient variants in the ankyrin repeat domain indicates there are DNA repair functions associated with this domain that have not been closely examined. In order to examine whether BARD1-associated loss of HDR function results in DNA damage sensitivity, cells expressing non-functional BARD1 variants were treated with ionizing radiation or cisplatin. These cells were found to be more sensitive to DNA damage, and variations in the residual HDR function of non-functional variants did not correlate with variations in sensitivity. These findings improve the understanding of BARD1 functional domains in DNA repair and support that this functional assay is useful for predicting the cancer association of BARD1 variants.
url http://europepmc.org/articles/PMC6457558?pdf=render
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