ASCO:趋化因子在预测t细胞炎症和对不同肿瘤类型免疫检查点抑制反应中的作用

2022-06-05 MedSci原创 MedSci原创

4个趋化因子组合有可能选择更广泛的可能受益于ICI的患者。

免疫检查点抑制剂(ICI)对某些癌症非常有效。新的T细胞炎症预测因子可能会识别出更广泛的具有ICI反应性的肿瘤子集。此前,来自加拿大McGill的学者已经确定了四个趋化因子(CCL4、CCL5、CXCL9、CXLC10)能够预测原发性和转移性胰腺肿瘤的T细胞炎症表型。

近期在ASCO2022大会上,该组学者进一步测试这4个趋化因子特征是否能预测其他类型肿瘤的T细胞炎症和对ICI的反应。研究人员利用来自癌症基因组图谱25种肿瘤类型的6455名患者的匹配基因组和转录组数据,搜索了4个趋化因子特征与抗肿瘤免疫力指标之间的关联。此外还测试了这一特征与DNA损伤修复缺陷标志物的关联。

大多数肿瘤类型显示出上述4个趋化因子和癌症-免疫循环的转录标志的高表达的亚群。睾丸生殖细胞瘤、宫颈鳞状细胞癌和头颈鳞状细胞癌是该特征的最强表达者。免疫调节基因,包括PD-L1、PD-1、TIM3、LAG3、TIGIT、CTLA-4和FASLG,在4个趋化因子队列中明显过度表达(P<0.05)。

参与癌症-免疫循环过程的基因组,包括MHC I的表达和细胞溶解活性,在4个趋化因子队列中被上调(P<0.05)。虽然肿瘤突变负担(TMB)和4个趋化因子的表达在整个肿瘤组织学类型中存在整体关系(rho=0.42,p=0.02),但高TMB仅与4个趋化因子肿瘤的一个子集有关。在接受ICI治疗的患者中,那些患有4个趋化因子肿瘤的患者的中位进展时间(104天对71天,p=0.013)和总生存期(391天对195天,p=0.016)更长。在预测总生存期方面,4个趋化因子特征的表现优于TMB。

综上,各种类型的肿瘤都存在T细胞炎症患者亚群,因此可能对ICI有良好的反应。4个趋化因子组合有可能选择更广泛的可能受益于ICI的患者。

 

参考文献:

Assessment of a 4-chemokine signature in prediction of T-cell inflammation and response to immune checkpoint inhibition across tumor types. First Author: Joan Miguel Romero, Research Institute of the McGill University Health Centre, Montreal, QC, Canada

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