Resolving the immune landscape of human prostate at a single-cell level in health and cancer

在健康和癌症状态下,从单细胞水平解析人类前列腺的免疫图谱

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作者:Zewen Kelvin Tuong ,Kevin W Loudon ,Brendan Berry ,Nathan Richoz ,Julia Jones ,Xiao Tan ,Quan Nguyen ,Anne George ,Satoshi Hori ,Sarah Field ,Andy G Lynch ,Katarzyna Kania ,Paul Coupland ,Anne Babbage ,Richard Grenfell ,Tristan Barrett ,Anne Y Warren ,Vincent Gnanapragasam ,Charlie Massie ,Menna R Clatworthy

Abstract

The prostate gland produces prostatic fluid, high in zinc and citrate and essential for the maintenance of spermatozoa. Prostate cancer is a common condition with limited treatment efficacy in castration-resistant metastatic disease, including with immune checkpoint inhibitors. Using single-cell RNA-sequencing to perform an unbiased assessment of the cellular landscape of human prostate, we identify a subset of tumor-enriched androgen receptor-negative luminal epithelial cells with increased expression of cancer-associated genes. We also find a variety of innate and adaptive immune cells in normal prostate that were transcriptionally perturbed in prostate cancer. An exception is a prostate-specific, zinc transporter-expressing macrophage population (MAC-MT) that contributes to tissue zinc accumulation in homeostasis but shows enhanced inflammatory gene expression in tumors, including T cell-recruiting chemokines. Remarkably, enrichment of the MAC-MT signature in cancer biopsies is associated with improved disease-free survival, suggesting beneficial antitumor functions.

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