A synergetic effect of BARD1 mutations on tumorigenesis

Wenjing Li; Xiaoyang Gu; Chunhong Liu; Yanyan Shi; Pan Wang; Na Zhang; Rui Wu; Liang Leng; Bingteng Xie; Chen Song; Mo Li

doi:10.1038/s41467-021-21519-3

A synergetic effect of BARD1 mutations on tumorigenesis

Wenjing Li
, Xiaoyang Gu
, Chunhong Liu
, Yanyan Shi
, Pan Wang
, Na Zhang
, Rui Wu
, Liang Leng
, Bingteng Xie
, Chen Song
, Mo Li^*

^*Corresponding author for this work

Peking University
China Academy of Chinese Medical Sciences

Research output: Contribution to journal › Article › peer-review

24 Citations (Scopus)

Abstract

To date, a large number of mutations have been screened from breast and ovarian cancer patients. However, most of them are classified into benign or unidentified alterations due to their undetectable phenotypes. Whether and how they could cause tumors remains unknown, and this significantly limits diagnosis and therapy. Here, in a study of a family with hereditary breast and ovarian cancer, we find that two BARD1 mutations, P24S and R378S, simultaneously exist in cis in surviving cancer patients. Neither of the single mutations causes a functional change, but together they synergetically impair the DNA damage response and lead to tumors in vitro and in vivo. Thus, our report not only demonstrates that BARD1 defects account for tumorigenesis but also uncovers the potential risk of synergetic effects between the large number of cis mutations in individual genes in the human genome.

Original language	English
Article number	1243
Journal	Nature Communications
Volume	12
Issue number	1
DOIs	https://doi.org/10.1038/s41467-021-21519-3
Publication status	Published - 1 Dec 2021
Externally published	Yes

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Cite this

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title = "A synergetic effect of BARD1 mutations on tumorigenesis",

abstract = "To date, a large number of mutations have been screened from breast and ovarian cancer patients. However, most of them are classified into benign or unidentified alterations due to their undetectable phenotypes. Whether and how they could cause tumors remains unknown, and this significantly limits diagnosis and therapy. Here, in a study of a family with hereditary breast and ovarian cancer, we find that two BARD1 mutations, P24S and R378S, simultaneously exist in cis in surviving cancer patients. Neither of the single mutations causes a functional change, but together they synergetically impair the DNA damage response and lead to tumors in vitro and in vivo. Thus, our report not only demonstrates that BARD1 defects account for tumorigenesis but also uncovers the potential risk of synergetic effects between the large number of cis mutations in individual genes in the human genome.",

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AU - Li, Wenjing

AU - Gu, Xiaoyang

AU - Liu, Chunhong

AU - Shi, Yanyan

AU - Wang, Pan

AU - Zhang, Na

AU - Wu, Rui

AU - Leng, Liang

AU - Xie, Bingteng

AU - Song, Chen

AU - Li, Mo

PY - 2021/12/1

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N2 - To date, a large number of mutations have been screened from breast and ovarian cancer patients. However, most of them are classified into benign or unidentified alterations due to their undetectable phenotypes. Whether and how they could cause tumors remains unknown, and this significantly limits diagnosis and therapy. Here, in a study of a family with hereditary breast and ovarian cancer, we find that two BARD1 mutations, P24S and R378S, simultaneously exist in cis in surviving cancer patients. Neither of the single mutations causes a functional change, but together they synergetically impair the DNA damage response and lead to tumors in vitro and in vivo. Thus, our report not only demonstrates that BARD1 defects account for tumorigenesis but also uncovers the potential risk of synergetic effects between the large number of cis mutations in individual genes in the human genome.

AB - To date, a large number of mutations have been screened from breast and ovarian cancer patients. However, most of them are classified into benign or unidentified alterations due to their undetectable phenotypes. Whether and how they could cause tumors remains unknown, and this significantly limits diagnosis and therapy. Here, in a study of a family with hereditary breast and ovarian cancer, we find that two BARD1 mutations, P24S and R378S, simultaneously exist in cis in surviving cancer patients. Neither of the single mutations causes a functional change, but together they synergetically impair the DNA damage response and lead to tumors in vitro and in vivo. Thus, our report not only demonstrates that BARD1 defects account for tumorigenesis but also uncovers the potential risk of synergetic effects between the large number of cis mutations in individual genes in the human genome.

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DO - 10.1038/s41467-021-21519-3

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VL - 12

JO - Nature Communications

JF - Nature Communications

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A synergetic effect of BARD1 mutations on tumorigenesis

Abstract

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