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A Subset of Localized Prostate Cancer Displays an Immunogenic Phenotype Associated with Losses of Key Tumor Suppressor Genes

前列腺癌 生物 癌症研究 CD8型 细胞毒性T细胞 免疫检查点 癌症 肿瘤微环境 祖细胞 T细胞 免疫系统 免疫学 免疫疗法 干细胞 遗传学 体外
作者
Carla Calagua,Miriam Ficial,Caroline S. Jansen,Taghreed Hirz,Luke del Balzo,Scott Wilkinson,Ross Lake,Anson T. Ku,Olga Voznesensky,David B. Sykes,Philip J. Saylor,Huihui Ye,Sabina Signoretti,Haydn Kissick,Adam G. Sowalsky,Steven P. Balk,David J. Einstein
出处
期刊:Clinical Cancer Research [American Association for Cancer Research]
卷期号:27 (17): 4836-4847 被引量:36
标识
DOI:10.1158/1078-0432.ccr-21-0121
摘要

Abstract Purpose: A subset of primary prostate cancer expresses programmed death-ligand 1 (PD-L1), but whether they have a unique tumor immune microenvironment or genomic features is unclear. Experimental Design: We selected PD-L1–positive high-grade and/or high-risk primary prostate cancer, characterized tumor-infiltrating lymphocytes with multiplex immunofluorescence, and identified genomic alterations in immunogenic and nonimmunogenic tumor foci. Results: One quarter of aggressive localized prostate cancer cases (29/115) had tumor PD-L1 expression more than 5%. This correlated with increased density of CD8+ T cells, a large fraction coexpressing PD-1, versus absent PD-1 expression on sparse CD8 T cells in unselected cases. Most CD8+PD-1+ cells did not express terminal exhaustion markers (TIM3 or LAG3), while a subset expressed TCF1. Consistent with these CD8+PD-1+TCF1+ cells being progenitors, they were found in antigen-presenting cell niches in close proximity to MHC-II+ cells. CD8 T-cell density in immunogenic prostate cancer and renal cell carcinoma (RCC) was nearly identical. Shallow RB1 and BRCA2 losses, and deep deletions of CHD1, were prevalent, the latter being strongly associated with a dendritic cell gene set in The Cancer Genome Atlas. Tumor mutation burden was variable; neither high microsatellite instability nor CDK12 alterations were present. Conclusions: A subset of localized prostate cancer is immunogenic, manifested by PD-L1 expression and CD8+ T-cell content comparable with RCC. The CD8+ T cells include effector cells and exhausted progenitor cells, which may be expanded by immune checkpoint inhibitors (ICI). Genomic losses of RB1, BRCA2, and CHD1 may be drivers of this phenotype. These findings indicate that immunotherapies may be effective in biomarker-selected subpopulations of patients with localized prostate cancer.
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