Identification of a comprehensive spectrum of genetic factors for hereditary breast cancer in a Chinese population by next-generation sequencing.

The genetic etiology of hereditary breast cancer has not been fully elucidated. Although germline mutations of high-penetrance genes such as BRCA1/2 are implicated in development of hereditary breast cancers, at least half of all breast cancer families are not linked to these genes. To identify a co...

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Main Authors: Xiaochen Yang, Jiong Wu, Jingsong Lu, Guangyu Liu, Genhong Di, Canming Chen, Yifeng Hou, Menghong Sun, Wentao Yang, Xiaojing Xu, Ying Zhao, Xin Hu, Daqiang Li, Zhigang Cao, Xiaoyan Zhou, Xiaoyan Huang, Zhebin Liu, Huan Chen, Yanzi Gu, Yayun Chi, Xia Yan, Qixia Han, Zhenzhou Shen, Zhimin Shao, Zhen Hu
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2015-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4415911?pdf=render
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spelling doaj-0902ef4acd924031a6a46be89f04b5512020-11-25T02:31:46ZengPublic Library of Science (PLoS)PLoS ONE1932-62032015-01-01104e012557110.1371/journal.pone.0125571Identification of a comprehensive spectrum of genetic factors for hereditary breast cancer in a Chinese population by next-generation sequencing.Xiaochen YangJiong WuJingsong LuGuangyu LiuGenhong DiCanming ChenYifeng HouMenghong SunWentao YangXiaojing XuYing ZhaoXin HuDaqiang LiZhigang CaoXiaoyan ZhouXiaoyan HuangZhebin LiuHuan ChenYanzi GuYayun ChiXia YanQixia HanZhenzhou ShenZhimin ShaoZhen HuThe genetic etiology of hereditary breast cancer has not been fully elucidated. Although germline mutations of high-penetrance genes such as BRCA1/2 are implicated in development of hereditary breast cancers, at least half of all breast cancer families are not linked to these genes. To identify a comprehensive spectrum of genetic factors for hereditary breast cancer in a Chinese population, we performed an analysis of germline mutations in 2,165 coding exons of 152 genes associated with hereditary cancer using next-generation sequencing (NGS) in 99 breast cancer patients from families of cancer patients regardless of cancer types. Forty-two deleterious germline mutations were identified in 21 genes of 34 patients, including 18 (18.2%) BRCA1 or BRCA2 mutations, 3 (3%) TP53 mutations, 5 (5.1%) DNA mismatch repair gene mutations, 1 (1%) CDH1 mutation, 6 (6.1%) Fanconi anemia pathway gene mutations, and 9 (9.1%) mutations in other genes. Of seven patients who carried mutations in more than one gene, 4 were BRCA1/2 mutation carriers, and their average onset age was much younger than patients with only BRCA1/2 mutations. Almost all identified high-penetrance gene mutations in those families fulfill the typical phenotypes of hereditary cancer syndromes listed in the National Comprehensive Cancer Network (NCCN) guidelines, except two TP53 and three mismatch repair gene mutations. Furthermore, functional studies of MSH3 germline mutations confirmed the association between MSH3 mutation and tumorigenesis, and segregation analysis suggested antagonism between BRCA1 and MSH3. We also identified a lot of low-penetrance gene mutations. Although the clinical significance of those newly identified low-penetrance gene mutations has not been fully appreciated yet, these new findings do provide valuable epidemiological information for the future studies. Together, these findings highlight the importance of genetic testing based on NCCN guidelines and a multi-gene analysis using NGS may be a supplement to traditional genetic counseling.http://europepmc.org/articles/PMC4415911?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Xiaochen Yang
Jiong Wu
Jingsong Lu
Guangyu Liu
Genhong Di
Canming Chen
Yifeng Hou
Menghong Sun
Wentao Yang
Xiaojing Xu
Ying Zhao
Xin Hu
Daqiang Li
Zhigang Cao
Xiaoyan Zhou
Xiaoyan Huang
Zhebin Liu
Huan Chen
Yanzi Gu
Yayun Chi
Xia Yan
Qixia Han
Zhenzhou Shen
Zhimin Shao
Zhen Hu
spellingShingle Xiaochen Yang
Jiong Wu
Jingsong Lu
Guangyu Liu
Genhong Di
Canming Chen
Yifeng Hou
Menghong Sun
Wentao Yang
Xiaojing Xu
Ying Zhao
Xin Hu
Daqiang Li
Zhigang Cao
Xiaoyan Zhou
Xiaoyan Huang
Zhebin Liu
Huan Chen
Yanzi Gu
Yayun Chi
Xia Yan
Qixia Han
Zhenzhou Shen
Zhimin Shao
Zhen Hu
Identification of a comprehensive spectrum of genetic factors for hereditary breast cancer in a Chinese population by next-generation sequencing.
PLoS ONE
author_facet Xiaochen Yang
Jiong Wu
Jingsong Lu
Guangyu Liu
Genhong Di
Canming Chen
Yifeng Hou
Menghong Sun
Wentao Yang
Xiaojing Xu
Ying Zhao
Xin Hu
Daqiang Li
Zhigang Cao
Xiaoyan Zhou
Xiaoyan Huang
Zhebin Liu
Huan Chen
Yanzi Gu
Yayun Chi
Xia Yan
Qixia Han
Zhenzhou Shen
Zhimin Shao
Zhen Hu
author_sort Xiaochen Yang
title Identification of a comprehensive spectrum of genetic factors for hereditary breast cancer in a Chinese population by next-generation sequencing.
title_short Identification of a comprehensive spectrum of genetic factors for hereditary breast cancer in a Chinese population by next-generation sequencing.
title_full Identification of a comprehensive spectrum of genetic factors for hereditary breast cancer in a Chinese population by next-generation sequencing.
title_fullStr Identification of a comprehensive spectrum of genetic factors for hereditary breast cancer in a Chinese population by next-generation sequencing.
title_full_unstemmed Identification of a comprehensive spectrum of genetic factors for hereditary breast cancer in a Chinese population by next-generation sequencing.
title_sort identification of a comprehensive spectrum of genetic factors for hereditary breast cancer in a chinese population by next-generation sequencing.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2015-01-01
description The genetic etiology of hereditary breast cancer has not been fully elucidated. Although germline mutations of high-penetrance genes such as BRCA1/2 are implicated in development of hereditary breast cancers, at least half of all breast cancer families are not linked to these genes. To identify a comprehensive spectrum of genetic factors for hereditary breast cancer in a Chinese population, we performed an analysis of germline mutations in 2,165 coding exons of 152 genes associated with hereditary cancer using next-generation sequencing (NGS) in 99 breast cancer patients from families of cancer patients regardless of cancer types. Forty-two deleterious germline mutations were identified in 21 genes of 34 patients, including 18 (18.2%) BRCA1 or BRCA2 mutations, 3 (3%) TP53 mutations, 5 (5.1%) DNA mismatch repair gene mutations, 1 (1%) CDH1 mutation, 6 (6.1%) Fanconi anemia pathway gene mutations, and 9 (9.1%) mutations in other genes. Of seven patients who carried mutations in more than one gene, 4 were BRCA1/2 mutation carriers, and their average onset age was much younger than patients with only BRCA1/2 mutations. Almost all identified high-penetrance gene mutations in those families fulfill the typical phenotypes of hereditary cancer syndromes listed in the National Comprehensive Cancer Network (NCCN) guidelines, except two TP53 and three mismatch repair gene mutations. Furthermore, functional studies of MSH3 germline mutations confirmed the association between MSH3 mutation and tumorigenesis, and segregation analysis suggested antagonism between BRCA1 and MSH3. We also identified a lot of low-penetrance gene mutations. Although the clinical significance of those newly identified low-penetrance gene mutations has not been fully appreciated yet, these new findings do provide valuable epidemiological information for the future studies. Together, these findings highlight the importance of genetic testing based on NCCN guidelines and a multi-gene analysis using NGS may be a supplement to traditional genetic counseling.
url http://europepmc.org/articles/PMC4415911?pdf=render
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