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Integrative molecular characterisation of gallbladder cancer reveals micro-environment-associated subtypes

胆囊癌 生物 转录组 外显子组测序 癌变 胆囊 外显子组 医学 癌症研究 癌症 内科学 突变 基因 遗传学 基因表达
作者
Chirag Nepal,Bin Zhu,Colm J. O’Rourke,Deepak Bhatt,Donghyuk Lee,Lei Song,Difei Wang,Alison L. Van Dyke,Hyoyoung Choo‐Wosoba,Zhiwei Liu,Allan Hildesheim,Alisa M. Goldstein,Michael Dean,Juan Lafuente-Barquero,Scott M. Lawrence,Karun Mutreja,Mary E. Olanich,Justo Lorenzo Bermejo,Catterina Ferreccio,Juan Carlos Roa,Asif Rashid,Ann W. Hsing,Yu‐Tang Gao,Stephen J. Chanock,J. C. Araya,Jesper B. Andersen,Jill Koshiol
出处
期刊:Journal of Hepatology [Elsevier BV]
卷期号:74 (5): 1132-1144 被引量:30
标识
DOI:10.1016/j.jhep.2020.11.033
摘要

Gallbladder cancer (GBC) is the most common type of biliary tract cancer, but the molecular mechanisms involved in gallbladder carcinogenesis remain poorly understood. In this study, we applied integrative genomics approaches to characterise GBC and explore molecular subtypes associated with patient survival.We profiled the mutational landscape of GBC tumours (whole-exome sequencing on 92, targeted sequencing on 98, in total 190 patients). In a subset (n = 45), we interrogated the matched transcriptomes, DNA methylomes, and somatic copy number alterations. We explored molecular subtypes identified through clustering tumours by genes whose expression was associated with survival in 47 tumours and validated subtypes on 34 publicly available GBC cases.Exome analysis revealed TP53 was the most mutated gene. The overall mutation rate was low (median 0.82 Mut/Mb). APOBEC-mediated mutational signatures were more common in tumours with higher mutational burden. Aflatoxin-related signatures tended to be highly clonal (present in ≥50% of cancer cells). Transcriptome-wide survival association analysis revealed a 95-gene signature that stratified all GBC patients into 3 subtypes that suggested an association with overall survival post-resection. The 2 poor-survival subtypes were associated with adverse clinicopathologic features (advanced stage, pN1, pM1), immunosuppressive micro-environments (myeloid-derived suppressor cell accumulation, extensive desmoplasia, hypoxia) and T cell dysfunction, whereas the good-survival subtype showed the opposite features.These data suggest that the tumour micro-environment and immune profiles could play an important role in gallbladder carcinogenesis and should be evaluated in future clinical studies, along with mutational profiles.Gallbladder cancer is highly fatal, and its causes are poorly understood. We evaluated gallbladder tumours to see if there were differences between tumours in genetic information such as DNA and RNA. We found evidence of aflatoxin exposure in these tumours, and immune cells surrounding the tumours were associated with survival.
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