Abstract | BACKGROUND:
Immunotherapy is considered as a powerful and promising clinical approach for the treatment of gastric cancer (GC). However, it is still challenging to precisely screen patients who potentially benefit from immune checkpoint therapy (ICT). Identification of potential biomarkers for selecting patients sensitive to immunotherapy was urgently needed. METHODS: Public sequence data and corresponding clinical data were used to explore the potential biomarkers for immunotherapy. RESULTS: We found that CSMD1 is the most frequently mutated gene and its mutation is highly correlated with prognosis in gastric cancer patients. Interestingly, patients with mutated CSMD1 exhibit a high mutation burden and upregulated PDL1 expression. The ratio of microsatellite instability (MSI) in the CSMD1 mutation cohort was higher than that in the cohort without CSMD1 mutation. Furthermore, patients with CSMD1 mutation have been found to possess a higher number of activated CD4+ T cells and neoantigens. CONCLUSION:
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Authors | Xuning Wang, Shixiang Wang, Yalin Han, Maolin Xu, Peng Li, Mu Ke, Zhipeng Teng, Pu Huang, Ziyan Diao, Yongfeng Yan, Qingyu Meng, Yanshen Kuang, Wei Zheng, Hongyi Liu, Xuesong Liu, Baoqing Jia |
Journal | International journal of general medicine
(Int J Gen Med)
Vol. 14
Pg. 8293-8299
( 2021)
ISSN: 1178-7074 [Print] New Zealand |
PMID | 34815701
(Publication Type: Journal Article)
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Copyright | © 2021 Wang et al. |