胃癌的多祖先基因组和转录组分析

Multiancestry genomic and transcriptomic analysis of gastric cancer.

作者信息

Totoki Yasushi, Saito-Adachi Mihoko, Shiraishi Yuichi, Komura Daisuke, Nakamura Hiromi, Suzuki Akihiro, Tatsuno Kenji, Rokutan Hirofumi, Hama Natsuko, Yamamoto Shogo, Ono Hanako, Arai Yasuhito, Hosoda Fumie, Katoh Hiroto, Chiba Kenichi, Iida Naoko, Nagae Genta, Ueda Hiroki, Shihang Chen, Sekine Shigeki, Abe Hiroyuki, Nomura Sachiyo, Matsuura Tetsuya, Sakai Eiji, Ohshima Takashi, Rino Yasushi, Yeoh Khay Guan, So Jimmy, Sanghvi Kaushal, Soong Richie, Fukagawa Akihiko, Yachida Shinichi, Kato Mamoru, Seto Yasuyuki, Ushiku Tetsuo, Nakajima Atsushi, Katai Hitoshi, Tan Patrick, Ishikawa Shumpei, Aburatani Hiroyuki, Shibata Tatsuhiro

机构信息

Division of Cancer Genomics, National Cancer Center Research Institute, Tokyo, Japan.

Division of Genome Analysis Platform Development, National Cancer Center Research Institute, Tokyo, Japan.

出版信息

Nat Genet. 2023 Apr;55(4):581-594. doi: 10.1038/s41588-023-01333-x. Epub 2023 Mar 13.

DOI:10.1038/s41588-023-01333-x

PMID:36914835

Abstract

Gastric cancer is among the most common malignancies worldwide, characterized by geographical, epidemiological and histological heterogeneity. Here, we report an extensive, multiancestral landscape of driver events in gastric cancer, involving 1,335 cases. Seventy-seven significantly mutated genes (SMGs) were identified, including ARHGAP5 and TRIM49C. We also identified subtype-specific drivers, including PIGR and SOX9, which were enriched in the diffuse subtype of the disease. SMGs also varied according to Epstein-Barr virus infection status and ancestry. Non-protein-truncating CDH1 mutations, which are characterized by in-frame splicing alterations, targeted localized extracellular domains and uniquely occurred in sporadic diffuse-type cases. In patients with gastric cancer with East Asian ancestry, our data suggested a link between alcohol consumption or metabolism and the development of RHOA mutations. Moreover, mutations with potential roles in immune evasion were identified. Overall, these data provide comprehensive insights into the molecular landscape of gastric cancer across various subtypes and ancestries.

摘要

胃癌是全球最常见的恶性肿瘤之一，具有地理、流行病学和组织学异质性。在此，我们报告了一项涉及1335例病例的广泛、多祖先的胃癌驱动事件图谱。鉴定出77个显著突变基因（SMG），包括ARHGAP5和TRIM49C。我们还鉴定出亚型特异性驱动基因，包括PIGR和SOX9，它们在该疾病的弥漫型亚型中富集。SMG也因爱泼斯坦-巴尔病毒感染状态和祖先不同而有所差异。非蛋白质截短的CDH1突变以框内剪接改变为特征，靶向局部细胞外结构域，且仅发生在散发性弥漫型病例中。在东亚血统的胃癌患者中，我们的数据表明饮酒或酒精代谢与RHOA突变的发生之间存在联系。此外，还鉴定出了在免疫逃逸中可能起作用的突变。总体而言，这些数据为不同亚型和祖先背景的胃癌分子图谱提供了全面的见解。

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胃癌的多祖先基因组和转录组分析

Multiancestry genomic and transcriptomic analysis of gastric cancer.

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