| Literature DB >> 35582821 |
Min Kyung Ju1, Joo Rak Lee1, Yeonsong Choi2, Seon Young Park3, Hee Jung Sul4, Hee Jin Chung1, Soyeong An1, Semin Lee2, Eunyoung Jung3, Bohyun Kim4, Bo Youn Choi4, Bum Jun Kim5, Hyeong Su Kim5, Hyun Lim5, Ho Suk Kang5, Jae Seung Soh5, Kyungjae Myung1,6, Kab Choong Kim7, Ji Woong Cho7, Jinwon Seo8, Tae Moon Kim6, Ja Yil Lee1,6, Yonghwan Kim3, Hongtae Kim1,6, Dae Young Zang4,5.
Abstract
Genome instability is one of the leading causes of gastric cancers. However, the mutational landscape of driver genes in gastric cancer is poorly understood. Here, we investigate somatic mutations in 25 Korean gastric adenocarcinoma patients using whole-exome sequencing and show that PWWP2B is one of the most frequently mutated genes. PWWP2B mutation correlates with lower cancer patient survival. We find that PWWP2B has a role in DNA double-strand break repair. As a nuclear protein, PWWP2B moves to sites of DNA damage through its interaction with UHRF1. Depletion of PWWP2B enhances cellular sensitivity to ionizing radiation (IR) and impairs IR-induced foci formation of RAD51. PWWP2B interacts with MRE11 and participates in homologous recombination via promoting DNA end-resection. Taken together, our data show that PWWP2B facilitates the recruitment of DNA repair machinery to sites of DNA damage and promotes HR-mediated DNA double-strand break repair. Impaired PWWP2B function might thus cause genome instability and promote gastric cancer development.Entities:
Keywords: PWWP2B; UHRF1; end resection; gastric cancer; homologous recombination
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Year: 2022 PMID: 35582821 PMCID: PMC9253748 DOI: 10.15252/embr.202153492
Source DB: PubMed Journal: EMBO Rep ISSN: 1469-221X Impact factor: 9.071