Identification of New Pathogenic Variants of Hereditary Diffuse Gastric Cancer

• Published in: Cancer research and treatment Vol. 56; no. 4; pp. 1126 - 1135
• Main Authors: Oh, Seung-Young, Jang, Giyong, Kim, Jaeryuk, Jeong, Kyoung-Yun, Kim, Hyun Myong, Kwak, Yoon Jin, Kong, Seong-Ho, Park, Do Joong, Lee, Hyuk-Joon, Cho, Sung-Yup, Kim, Jong-Il, Yang, Han-Kwang
• Format: Journal Article
• Language: English
• Published: Korea (South) Korean Cancer Association 01.10.2024; 대한암학회
• Subjects: Original; 의학일반; Pathogenic variant; Hereditary diffuse gastric cancer; Familial gastric cancer; Germ-Line mutation; RHOA
• ISSN: 1598-2998; 2005-9256; 2005-9256
• DOI: 10.4143/crt.2024.328

Purpose Hereditary diffuse gastric cancer (HDGC) presents a significant genetic predisposition, notably linked to mutations in the CDH1 and CTNNA1. However, the genetic basis for over half of HDGC cases remains unidentified. The aim of this study is to identify novel pathogenic variants in HDGC and evaluate their protein expression.Materials and Methods Among 20 qualifying families, two were selected based on available pedigree and DNA. Whole genome sequencing (WGS) on DNA extracted from blood and whole exome sequencing on DNA from formalin-fixed paraffin-embedded tissues were performed to find potential pathogenic variants in HDGC. After selection of a candidate variant, functional validation, and enrichment analysis were performed.Results As a result of WGS, three candidate germline mutations (EPHA5, MCOA2, and RHOA) were identified in one family. After literature review and in-silico analyses, the RHOA mutation (R129W) was selected as a candidate. This mutation was found in two gastric cancer patients within the family. In functional validation, it showed RhoA overexpression and a higher GTP-bound state in the RhoaR129W mutant. Decreased phosphorylation at Ser127/397 suggested altered YAP1 regulation in the Rho-ROCK pathway. Gene Ontology (GO) and Kyoto Encyclopedia of Genes and Genomes (KEGG) analyses linked RhoaR129W overexpression to changed migration/adhesion in MKN1 cell line. However, this RHOA mutation (R129W) was not found in index patients in other families.Conclusion The RHOA mutation (R129W) emerges as a potential causative gene for HDGC, but only in one family, indicating a need for further studies to understand its role in HDGC pathogenesis fully.