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Functional consequences of a rare missense BARD1 c.403G>A germline mutation identified in a triple-negative breast cancer patient.


ABSTRACT: We identified a rare missense germline mutation in BARD1 (c.403G>A or p.Asp135Asn) as pathogenic using integrated genomics and transcriptomics profiling of germline and tumor samples from an early-onset triple-negative breast cancer patient who later was administrated with a PARP inhibitor for 2 months. We demonstrated in cell and mouse models that, compared to the wild-type, (1) c.403G>A mutant cell lines were more sensitive to irradiation, a DNA damage agent, and a PARP inhibitor; (2) c.403G>A mutation inhibited interaction between BARD1 and RAD51 (but not BRCA1); and (3) c.403G>A mutant mice were hypersensitive to ionizing radiation. Our study shed lights on the clinical interpretation of rare germline mutations of BARD1.

SUBMITTER: Zheng Y 

PROVIDER: S-EPMC8088670 | biostudies-literature | 2021 May

REPOSITORIES: biostudies-literature

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Functional consequences of a rare missense BARD1 c.403G>A germline mutation identified in a triple-negative breast cancer patient.

Zheng Yuanting Y   Li Bingying B   Pan Dejing D   Cao Jun J   Zhang Jian J   Wang Xiaolin X   Li Xiangnan X   Hou Wanwan W   Bao Ding D   Ren Luyao L   Yang Jingcheng J   Wang Shangzi S   Qiu Yangyang Y   Zhou Fei F   Liu Zhiwei Z   Zhu Sibo S   Zhang Lei L   Qing Tao T   Wang Yi Y   Yu Ying Y   Wu Jiaxue J   Hu Xichun X   Shi Leming L  

Breast cancer research : BCR 20210501 1


We identified a rare missense germline mutation in BARD1 (c.403G>A or p.Asp135Asn) as pathogenic using integrated genomics and transcriptomics profiling of germline and tumor samples from an early-onset triple-negative breast cancer patient who later was administrated with a PARP inhibitor for 2 months. We demonstrated in cell and mouse models that, compared to the wild-type, (1) c.403G>A mutant cell lines were more sensitive to irradiation, a DNA damage agent, and a PARP inhibitor; (2) c.403G>A  ...[more]

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