| Literature DB >> 35121863 |
Yosuke Tanaka1, Fumiko Chiwaki2, Shinya Kojima3, Masahito Kawazu3, Masayuki Komatsu2, Toshihide Ueno3, Satoshi Inoue3, Shigeki Sekine4, Keisuke Matsusaki5, Hiromichi Matsushita6, Narikazu Boku7, Yae Kanai8, Yasushi Yatabe4, Hiroki Sasaki9, Hiroyuki Mano10.
Abstract
Peritoneal metastasis, a hallmark of incurable advanced gastric cancer (GC), presently has no curative therapy and its molecular features have not been examined extensively. Here we present a comprehensive multi-omic analysis of malignant ascitic fluid samples and their corresponding tumor cell lines from 98 patients, including whole-genome sequencing, RNA sequencing, DNA methylation and enhancer landscape. We identify a higher frequency of receptor tyrosine kinase and mitogen-activated protein kinase pathway alterations compared to primary GC; moreover, approximately half of the gene alterations are potentially treatable with targeted therapy. Our analyses also stratify ascites-disseminated GC into two distinct molecular subtypes: one displaying active super enhancers (SEs) at the ELF3, KLF5 and EHF loci, and a second subtype bearing transforming growth factor-β (TGF-β) pathway activation through SMAD3 SE activation and high expression of transcriptional enhancer factor TEF-1 (TEAD1). In the TGF-β subtype, inhibition of the TEAD pathway circumvents therapy resistance, suggesting a potential molecular-guided therapeutic strategy for this subtype of intractable GC.Entities:
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Year: 2021 PMID: 35121863 DOI: 10.1038/s43018-021-00240-6
Source DB: PubMed Journal: Nat Cancer ISSN: 2662-1347