Intratumoral CD4+ T Cells Mediate Anti-tumor Cytotoxicity in Human Bladder Cancer

肿瘤内CD4+ T细胞介导人膀胱癌的抗肿瘤细胞毒性

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作者:David Y Oh ,Serena S Kwek ,Siddharth S Raju ,Tony Li ,Elizabeth McCarthy ,Eric Chow ,Dvir Aran ,Arielle Ilano ,Chien-Chun Steven Pai ,Chiara Rancan ,Kathryn Allaire ,Arun Burra ,Yang Sun ,Matthew H Spitzer ,Serghei Mangul ,Sima Porten ,Maxwell V Meng ,Terence W Friedlander ,Chun Jimmie Ye ,Lawrence Fong

Abstract

Responses to anti-PD-1 immunotherapy occur but are infrequent in bladder cancer. The specific T cells that mediate tumor rejection are unknown. T cells from human bladder tumors and non-malignant tissue were assessed with single-cell RNA and paired T cell receptor (TCR) sequencing of 30,604 T cells from 7 patients. We find that the states and repertoires of CD8+ T cells are not distinct in tumors compared with non-malignant tissues. In contrast, single-cell analysis of CD4+ T cells demonstrates several tumor-specific states, including multiple distinct states of regulatory T cells. Surprisingly, we also find multiple cytotoxic CD4+ T cell states that are clonally expanded. These CD4+ T cells can kill autologous tumors in an MHC class II-dependent fashion and are suppressed by regulatory T cells. Further, a gene signature of cytotoxic CD4+ T cells in tumors predicts a clinical response in 244 metastatic bladder cancer patients treated with anti-PD-L1. Trial registration: ClinicalTrials.gov NCT02451423.

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