FAT4 mutation as a potential predictive biomarker for immunotherapy combined with anti-angiogenic therapy in MSS metastatic colorectal cancer.

医学 结直肠癌 内科学 肿瘤科 免疫疗法 精确检验 微卫星不稳定性 癌症 微卫星 基因 生物 等位基因 生物化学
作者
Mifen Chen,Qi Zhang,H. S. Chen,Zhenghang Wang,Ting Xu,Changsong Qi,Shiqing Chen,Xiaochen Zhao,Yuezong Bai,Zhi Peng,Xicheng Wang,Xiaotian Zhang,Jifang Gong,Lin Shen,Jian Li
出处
期刊:Journal of Clinical Oncology [American Society of Clinical Oncology]
卷期号:40 (16_suppl): e15504-e15504 被引量:1
标识
DOI:10.1200/jco.2022.40.16_suppl.e15504
摘要

e15504 Background: Microsatellite stable (MSS) metastatic colorectal cancer (CRC) lacks effective treatments and has a poor prognosis. The aim of this study was to identify patients who could benefit from immunotherapy combined with anti-angiogenic therapy. Exploration of predictive biomarkers could help to maximize the clinical benefits. Methods: In total, FFPE tissues samples before immunotherapy combined with anti-angiogenic therapy of 21 patients were successfully tested for tumor microenvironments (TMEs) by multiple immunofluorescence, of which 11 of them were successfully detected by 733-gene NGS panel in a CLIA-certified laboratory. The correlation between gene variations and clinical durable benefit (DCB: PR, or SD≥6 months), PFS and TMEs were analyzed by Fisher's test, K-M survival curve analysis and Mann Whitney analysis respectively. Results: Significant difference was detected between FAT4 mutation (FAT4-MUT) and FAT4 wildtype (FAT4-WT) regarding DCB (100%, 4/4 vs 17%, 1/7, P = 0.0152) and progress-free survival (median PFS, 13.8 months vs 2.8 months, LogRank P = 0.003). There was no significant difference in TMB level between DCB and NDB (SD<6 months, or PD) groups (12 mut/Mb vs 6 mut/Mb, P = 0.0823) or between FAT4-MUT and FAT4-WT (11 mut/Mb vs 6 mut/Mb, P = 0.3697). TMEs analyses revealed that the CD3+CD4+ T cell proportion was tended to be higher in FAT4-MUT (0.7% vs 0.3%, P = 0.054). Further TIMER2.0 data showed FAT4-MUT was significantly associated with higher Immune infiltration of four immune cells, including CD4+ T cell in both colon and rectal adenocarcinoma, CD8+ central memory T cell, B cell, and Macrophage in colon adenocarcinoma. Conclusions: Our findings indicated that FAT4 mutation serves as a potential novel biomarker correlated with a better response to immunotherapy combined with anti-angiogenic therapy in MSS metastatic CRC, which may be related to the activation of CD4 T cell infiltration. However, these need to be validated by further cohort expansion.
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