T‐cell lymphoma patient harboring BCL11B mutations had favorable overall survival

危险系数 错义突变 突变 淋巴瘤 肿瘤科 癌症研究 生物 内科学 遗传学 医学 基因 置信区间
作者
Cunte Chen,Ling Huang,Sichu Liu,Xingshan Jiang,Feili Chen,Xiaojuan Wei,Hanguo Guo,Xiangbo Zeng,Chengwu Zeng,Grzegorz K. Przybylski,Wenyu Li,Yangqiu Li
出处
期刊:Asia-pacific Journal of Clinical Oncology [Wiley]
被引量:1
标识
DOI:10.1111/ajco.14000
摘要

Abstract Background Molecular genetics serve a critical role in constructing risk stratification for hematological malignancies, but T‐cell lymphoma (TCL) still lacks molecular genetic information for supplement risk stratification in predicting the prognosis of TCL patients. In the present study, we characterized the mutation patterns of B‐cell leukemia/lymphoma 11B gene ( BCL11B ) and its prognostic importance in TCL patients. Methods BCL11B mutations were characterized based on the data from two datasets, one is from our clinical center (GDPH dataset, n = 79) and the other is from COSMIC dataset ( n = 154). Results The overall mutation rate of BCL11B was 6.4% (15/233) in TCL, and there were no hotspot mutation sites in TCL. Among these mutations, the missense and splice site mutation were significantly prominent. Moreover, TCL patients harboring BCL11B mutations had a favorable overall survival (OS) in our center (GDPH dataset) (adjusted hazard ratio [HR] = .001, p = 0.109), although there were not yet significantly statistical at this point. In addition, TCL patients harboring BCL11B mutation had a longer 5‐year restricted mean survival time (RMST) than those without a BCL11B mutation (60 vs. 32 months). Notably, BCL11B mutations were not associated with TCL entities having better prognosis. Conclusions BCL11B mutations were associated with favorable clinical outcome for TCL patients; it might be considered as a novel biomarker for TCL prognostic stratification.
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