Genomic Analyses Reveal Mutational Signatures and Frequently Altered Genes in Esophageal Squamous Cell Carcinoma

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Esophageal squamous cell carcinoma (ESCC) is one of the most common cancers worldwide and the fourth most lethal cancer in China. However, although genomic studies have identified some mutations associated with ESCC, we know little of the mutational processes responsible. To identify genome-wide mut...

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Autores principales: Zhang, Ling, Zhou, Yong, Cheng, Caixia, Cui, Heyang, Cheng, Le, Kong, Pengzhou, Wang, Jiaqian, Li, Yin, Chen, Wenliang, Song, Bin, Wang, Fang, Jia, Zhiwu, Li, Lin, Li, Yaoping, Yang, Bin, Liu, Jing, Shi, Ruyi, Bi, Yanghui, Zhang, Yanyan, Wang, Juan, Zhao, Zhenxiang, Hu, Xiaoling, Yang, Jie, Li, Hongyi, Gao, Zhibo, Chen, Gang, Huang, Xuanlin, Yang, Xukui, Wan, Shengqing, Chen, Chao, Li, Bin, Tan, Yongkai, Chen, Longyun, He, Minghui, Xie, Sha, Li, Xiangchun, Zhuang, Xuehan, Wang, Mengyao, Xia, Zhi, Luo, Longhai, Ma, Jie, Dong, Bing, Zhao, Jiuzhou, Song, Yongmei, Ou, Yunwei, Li, Enming, Xu, Liyan, Wang, Jinfen, Xi, Yanfeng, Li, Guodong, Xu, Enwei, Liang, Jianfang, Yang, Xiaofeng, Guo, Jiansheng, Chen, Xing, Zhang, Yanbo, Li, Qingshan, Liu, Lixin, Li, Yingrui, Zhang, Xiuqing, Yang, Huanming, Lin, Dongxin, Cheng, Xiaolong, Guo, Yongjun, Wang, Jun, Zhan, Qimin, Cui, Yongping
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2015
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4385186/
https://www.ncbi.nlm.nih.gov/pubmed/25839328
http://dx.doi.org/10.1016/j.ajhg.2015.02.017
_version_ 1782365021905354752
author Zhang, Ling
Zhou, Yong
Cheng, Caixia
Cui, Heyang
Cheng, Le
Kong, Pengzhou
Wang, Jiaqian
Li, Yin
Chen, Wenliang
Song, Bin
Wang, Fang
Jia, Zhiwu
Li, Lin
Li, Yaoping
Yang, Bin
Liu, Jing
Shi, Ruyi
Bi, Yanghui
Zhang, Yanyan
Wang, Juan
Zhao, Zhenxiang
Hu, Xiaoling
Yang, Jie
Li, Hongyi
Gao, Zhibo
Chen, Gang
Huang, Xuanlin
Yang, Xukui
Wan, Shengqing
Chen, Chao
Li, Bin
Tan, Yongkai
Chen, Longyun
He, Minghui
Xie, Sha
Li, Xiangchun
Zhuang, Xuehan
Wang, Mengyao
Xia, Zhi
Luo, Longhai
Ma, Jie
Dong, Bing
Zhao, Jiuzhou
Song, Yongmei
Ou, Yunwei
Li, Enming
Xu, Liyan
Wang, Jinfen
Xi, Yanfeng
Li, Guodong
Xu, Enwei
Liang, Jianfang
Yang, Xiaofeng
Guo, Jiansheng
Chen, Xing
Zhang, Yanbo
Li, Qingshan
Liu, Lixin
Li, Yingrui
Zhang, Xiuqing
Yang, Huanming
Lin, Dongxin
Cheng, Xiaolong
Guo, Yongjun
Wang, Jun
Zhan, Qimin
Cui, Yongping
author_facet Zhang, Ling
Zhou, Yong
Cheng, Caixia
Cui, Heyang
Cheng, Le
Kong, Pengzhou
Wang, Jiaqian
Li, Yin
Chen, Wenliang
Song, Bin
Wang, Fang
Jia, Zhiwu
Li, Lin
Li, Yaoping
Yang, Bin
Liu, Jing
Shi, Ruyi
Bi, Yanghui
Zhang, Yanyan
Wang, Juan
Zhao, Zhenxiang
Hu, Xiaoling
Yang, Jie
Li, Hongyi
Gao, Zhibo
Chen, Gang
Huang, Xuanlin
Yang, Xukui
Wan, Shengqing
Chen, Chao
Li, Bin
Tan, Yongkai
Chen, Longyun
He, Minghui
Xie, Sha
Li, Xiangchun
Zhuang, Xuehan
Wang, Mengyao
Xia, Zhi
Luo, Longhai
Ma, Jie
Dong, Bing
Zhao, Jiuzhou
Song, Yongmei
Ou, Yunwei
Li, Enming
Xu, Liyan
Wang, Jinfen
Xi, Yanfeng
Li, Guodong
Xu, Enwei
Liang, Jianfang
Yang, Xiaofeng
Guo, Jiansheng
Chen, Xing
Zhang, Yanbo
Li, Qingshan
Liu, Lixin
Li, Yingrui
Zhang, Xiuqing
Yang, Huanming
Lin, Dongxin
Cheng, Xiaolong
Guo, Yongjun
Wang, Jun
Zhan, Qimin
Cui, Yongping
author_sort Zhang, Ling
collection PubMed
description Esophageal squamous cell carcinoma (ESCC) is one of the most common cancers worldwide and the fourth most lethal cancer in China. However, although genomic studies have identified some mutations associated with ESCC, we know little of the mutational processes responsible. To identify genome-wide mutational signatures, we performed either whole-genome sequencing (WGS) or whole-exome sequencing (WES) on 104 ESCC individuals and combined our data with those of 88 previously reported samples. An APOBEC-mediated mutational signature in 47% of 192 tumors suggests that APOBEC-catalyzed deamination provides a source of DNA damage in ESCC. Moreover, PIK3CA hotspot mutations (c.1624G>A [p.Glu542Lys] and c.1633G>A [p.Glu545Lys]) were enriched in APOBEC-signature tumors, and no smoking-associated signature was observed in ESCC. In the samples analyzed by WGS, we identified focal (<100 kb) amplifications of CBX4 and CBX8. In our combined cohort, we identified frequent inactivating mutations in AJUBA, ZNF750, and PTCH1 and the chromatin-remodeling genes CREBBP and BAP1, in addition to known mutations. Functional analyses suggest roles for several genes (CBX4, CBX8, AJUBA, and ZNF750) in ESCC. Notably, high activity of hedgehog signaling and the PI3K pathway in approximately 60% of 104 ESCC tumors indicates that therapies targeting these pathways might be particularly promising strategies for ESCC. Collectively, our data provide comprehensive insights into the mutational signatures of ESCC and identify markers for early diagnosis and potential therapeutic targets.
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spelling pubmed-43851862015-07-10 Genomic Analyses Reveal Mutational Signatures and Frequently Altered Genes in Esophageal Squamous Cell Carcinoma Zhang, Ling Zhou, Yong Cheng, Caixia Cui, Heyang Cheng, Le Kong, Pengzhou Wang, Jiaqian Li, Yin Chen, Wenliang Song, Bin Wang, Fang Jia, Zhiwu Li, Lin Li, Yaoping Yang, Bin Liu, Jing Shi, Ruyi Bi, Yanghui Zhang, Yanyan Wang, Juan Zhao, Zhenxiang Hu, Xiaoling Yang, Jie Li, Hongyi Gao, Zhibo Chen, Gang Huang, Xuanlin Yang, Xukui Wan, Shengqing Chen, Chao Li, Bin Tan, Yongkai Chen, Longyun He, Minghui Xie, Sha Li, Xiangchun Zhuang, Xuehan Wang, Mengyao Xia, Zhi Luo, Longhai Ma, Jie Dong, Bing Zhao, Jiuzhou Song, Yongmei Ou, Yunwei Li, Enming Xu, Liyan Wang, Jinfen Xi, Yanfeng Li, Guodong Xu, Enwei Liang, Jianfang Yang, Xiaofeng Guo, Jiansheng Chen, Xing Zhang, Yanbo Li, Qingshan Liu, Lixin Li, Yingrui Zhang, Xiuqing Yang, Huanming Lin, Dongxin Cheng, Xiaolong Guo, Yongjun Wang, Jun Zhan, Qimin Cui, Yongping Am J Hum Genet Article Esophageal squamous cell carcinoma (ESCC) is one of the most common cancers worldwide and the fourth most lethal cancer in China. However, although genomic studies have identified some mutations associated with ESCC, we know little of the mutational processes responsible. To identify genome-wide mutational signatures, we performed either whole-genome sequencing (WGS) or whole-exome sequencing (WES) on 104 ESCC individuals and combined our data with those of 88 previously reported samples. An APOBEC-mediated mutational signature in 47% of 192 tumors suggests that APOBEC-catalyzed deamination provides a source of DNA damage in ESCC. Moreover, PIK3CA hotspot mutations (c.1624G>A [p.Glu542Lys] and c.1633G>A [p.Glu545Lys]) were enriched in APOBEC-signature tumors, and no smoking-associated signature was observed in ESCC. In the samples analyzed by WGS, we identified focal (<100 kb) amplifications of CBX4 and CBX8. In our combined cohort, we identified frequent inactivating mutations in AJUBA, ZNF750, and PTCH1 and the chromatin-remodeling genes CREBBP and BAP1, in addition to known mutations. Functional analyses suggest roles for several genes (CBX4, CBX8, AJUBA, and ZNF750) in ESCC. Notably, high activity of hedgehog signaling and the PI3K pathway in approximately 60% of 104 ESCC tumors indicates that therapies targeting these pathways might be particularly promising strategies for ESCC. Collectively, our data provide comprehensive insights into the mutational signatures of ESCC and identify markers for early diagnosis and potential therapeutic targets. Elsevier 2015-04-02 /pmc/articles/PMC4385186/ /pubmed/25839328 http://dx.doi.org/10.1016/j.ajhg.2015.02.017 Text en © 2015 The Authors http://creativecommons.org/licenses/by-nc-nd/3.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/3.0/).
spellingShingle Article
Zhang, Ling
Zhou, Yong
Cheng, Caixia
Cui, Heyang
Cheng, Le
Kong, Pengzhou
Wang, Jiaqian
Li, Yin
Chen, Wenliang
Song, Bin
Wang, Fang
Jia, Zhiwu
Li, Lin
Li, Yaoping
Yang, Bin
Liu, Jing
Shi, Ruyi
Bi, Yanghui
Zhang, Yanyan
Wang, Juan
Zhao, Zhenxiang
Hu, Xiaoling
Yang, Jie
Li, Hongyi
Gao, Zhibo
Chen, Gang
Huang, Xuanlin
Yang, Xukui
Wan, Shengqing
Chen, Chao
Li, Bin
Tan, Yongkai
Chen, Longyun
He, Minghui
Xie, Sha
Li, Xiangchun
Zhuang, Xuehan
Wang, Mengyao
Xia, Zhi
Luo, Longhai
Ma, Jie
Dong, Bing
Zhao, Jiuzhou
Song, Yongmei
Ou, Yunwei
Li, Enming
Xu, Liyan
Wang, Jinfen
Xi, Yanfeng
Li, Guodong
Xu, Enwei
Liang, Jianfang
Yang, Xiaofeng
Guo, Jiansheng
Chen, Xing
Zhang, Yanbo
Li, Qingshan
Liu, Lixin
Li, Yingrui
Zhang, Xiuqing
Yang, Huanming
Lin, Dongxin
Cheng, Xiaolong
Guo, Yongjun
Wang, Jun
Zhan, Qimin
Cui, Yongping
Genomic Analyses Reveal Mutational Signatures and Frequently Altered Genes in Esophageal Squamous Cell Carcinoma
title Genomic Analyses Reveal Mutational Signatures and Frequently Altered Genes in Esophageal Squamous Cell Carcinoma
title_full Genomic Analyses Reveal Mutational Signatures and Frequently Altered Genes in Esophageal Squamous Cell Carcinoma
title_fullStr Genomic Analyses Reveal Mutational Signatures and Frequently Altered Genes in Esophageal Squamous Cell Carcinoma
title_full_unstemmed Genomic Analyses Reveal Mutational Signatures and Frequently Altered Genes in Esophageal Squamous Cell Carcinoma
title_short Genomic Analyses Reveal Mutational Signatures and Frequently Altered Genes in Esophageal Squamous Cell Carcinoma
title_sort genomic analyses reveal mutational signatures and frequently altered genes in esophageal squamous cell carcinoma
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4385186/
https://www.ncbi.nlm.nih.gov/pubmed/25839328
http://dx.doi.org/10.1016/j.ajhg.2015.02.017
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