Whole-exome Sequencing Reveals New Potential Susceptibility Genes for Japanese Familial Pancreatic Cancer

杂合子丢失 克拉斯 生殖系 种系突变 医学 外显子组测序 胰腺癌 外显子组 癌变 体细胞 基因 人口 生物 遗传学 癌症 癌症研究 突变 等位基因 环境卫生
作者
Erina Takai,Hiromi Nakamura,Suenori Chiku,Emi Kubo,Akihiro Ohmoto,Yasushi Totoki,Tatsuhiro Shibata,Ryota Higuchi,Masakazu Yamamoto,Junji Furuse,Kyoko Shimizu,Hideaki Takahashi,Chigusa Morizane,Toru Furukawa,Shinichi Yachida
出处
期刊:Annals of Surgery [Ovid Technologies (Wolters Kluwer)]
卷期号:275 (4): e652-e658 被引量:17
标识
DOI:10.1097/sla.0000000000004213
摘要

Objective: The primary objective of this study was to identify novel genes that predispose people in the Japanese population to FPC. Summary of Background Data: Familial history of pancreatic cancer is an important risk factor but, to date, few genes predisposing individuals to increased risk of developing FPC have been identified. Methods: We performed whole-exome sequencing of germline DNA from 81 Japanese FPC patients. We also investigated somatic gene alterations in 21 matched tumor tissues through whole-exome sequencing and copy number analysis. Results: Our germline variants identified previously known FPC susceptibility genes such as ATM and BRCA2 , and several novel tumor suppressor genes with potentially deleterious variants for FPC. Interestingly, somatic whole-exome analysis demonstrated that most tumor samples with suspicious loss of heterozygosity of candidate genes were KRAS wild-types, implying that these cases may not have required KRAS activation as a driver event for carcinogenesis. Conclusions: Our findings indicate that FPC patients harbor potentially deleterious causative germline variants in tumor suppressor genes, which are known to acquire somatic mutations in pancreatic cancer, and that somatic loss of heterozygosity of some FPC susceptibility genes may contribute to the development of FPC in the absence of somatic KRAS -activating mutation. Genetic testing for a wider variety of FPC-predisposition genes could provide better screening approach for high-risk groups of pancreatic cancer.
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