PTPRD/PTPRT突变与泛癌免疫治疗结果和免疫景观相关

Gangjian Wang, Xin Ji, Haojie Wang, Xiaohuan Tang, Xiaofang Xing, Jiafu Ji
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摘要

目的:PTPRD和PTPRT是与免疫治疗相关的JAK-STAT通路的磷酸酶。然而,PTPRD和PTPRT突变在多种癌症中的作用和机制尚不清楚。方法:收集12个队列的临床资料和PTPRD/PTPRT突变信息,分为发现队列和验证队列。分析PTPRD/PTPRT突变与免疫治疗疗效的关系。然后,使用癌症基因组图谱(TCGA)队列分析PTPRD/PTPRT突变与免疫谱之间的关系。结果:共有20种癌症类型的2392名患者被纳入本研究。我们的研究结果表明,携带PTPRD/PTPRT突变的患者,特别是共突变的患者,对多种癌症的免疫治疗反应率显著提高。PTPRD/PTPRT突变患者客观缓解率(ORR)较高(P=0.002),总生存期(OS)较长(P=0.005),无进展生存期(PFS)较长(P=0.038)。重要的是,上述发现在验证队列中得到了进一步验证。此外,我们发现PTPRD/PTPRT共突变(co-mut)亚组表现出免疫激活表型,野生型亚组倾向于免疫荒漠表型,而单突变(unit -mut)亚组可能具有免疫混合表型。我们进一步的分析表明,结合程序性细胞死亡配体1 (PD-L1)表达和PTPRD/PTPRT突变可用于筛选可能受益于免疫治疗的患者。结论:PTPRD/PTPRT突变可作为癌症免疫治疗的潜在预测性生物标志物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
PTPRD/PTPRT mutation correlates to treatment outcomes of immunotherapy and immune landscape in pan-cancers.

Objective: PTPRD and PTPRT are phosphatases of the JAK-STAT pathway related to immunotherapy. However, the role and mechanism of PTPRD and PTPRT mutations in multiple cancers remains unclear.

Methods: Clinical data and PTPRD/PTPRT mutation information from 12 cohorts were collected and classified as a discovery cohort and three validation cohorts. The association between PTPRD/PTPRT mutations and immunotherapeutic efficacy was analyzed. Then, the association between PTPRD/PTPRT mutation and immune profiles was analyzed using The Cancer Genome Atlas (TCGA) cohort.

Results: A total of 2,392 patients across 20 cancer types were included in this study. Our results showed that patients harboring PTPRD/PTPRT mutation, especially co-mutations, had a significantly elevated response rate to immunotherapy in multiple cancers. Patients with PTPRD/PTPRT mutation had a higher objective response rate (ORR) (P=0.002), longer overall survival (OS) (P=0.005) and progression-free survival (PFS) (P=0.038). Importantly, the above findings were further verified in validation cohorts. In addition, we found that the PTPRD/PTPRT co-mutations (co-mut) subgroup exhibited an immune-activated phenotype, the wild-type subgroup tended to have an immune-desert phenotype, and the uni-mutation (uni-mut) subgroup might have an immune-mixed phenotype. Our further analyses suggested that combining programmed cell death ligand 1 (PD-L1) expression and PTPRD/PTPRT mutation can be used to screen patients who may benefit from immunotherapy.

Conclusions: PTPRD/PTPRT mutation could serve as a potential predictive biomarker for cancer immunotherapy.

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