PROSTATE CELL HETEROGENEITY AND CXCL17 UPREGULATION IN MOUSE STEROID HORMONE IMBALANCE

Samara V Silver; Kayah J Tucker; Renee E Vickman; Nadia A Lanman; O John Semmes; Nehemiah S Alvarez; Petra Popovics

doi:10.1101/2024.04.24.590980

PROSTATE CELL HETEROGENEITY AND CXCL17 UPREGULATION IN MOUSE STEROID HORMONE IMBALANCE

bioRxiv [Preprint]. 2024 Apr 28:2024.04.24.590980. doi: 10.1101/2024.04.24.590980.

Authors

Samara V Silver^{1

2}, Kayah J Tucker^{1

2}, Renee E Vickman³, Nadia A Lanman^{4

5}, O John Semmes^{1

2}, Nehemiah S Alvarez³, Petra Popovics^{1

2}

Affiliations

¹ Department of Microbiology and Molecular Cell Biology, Eastern Virginia Medical School, Norfolk, VA.
² Leroy T. Canoles Jr. Cancer Research Center, Eastern Virginia Medical School, Norfolk, VA.
³ Department of Surgery, Endeavor Health, an Academic Affiliate of the University of Chicago Pritzker School of Medicine, Evanston, IL, USA.
⁴ Institute for Cancer Research, Purdue University, West Lafayette, IN, USA.
⁵ Department of Comparative Pathobiology, Purdue University, West Lafayette, IN, USA.

Abstract

Benign prostatic hyperplasia (BPH) is a prevalent age-related condition often characterized by debilitating urinary symptoms. Its etiology is believed to stem from hormonal imbalance, particularly an elevated estradiol-to-testosterone ratio and chronic inflammation. Our previous studies using a mouse steroid hormone imbalance model identified a specific increase in macrophages that migrate and accumulate in the prostate lumen where they differentiate into lipid-laden foam cells in mice implanted with testosterone and estradiol pellets, but not in sham animals. The current study focused on further characterizing the cellular heterogeneity of the prostate in this model as well as identifying the specific transcriptomic signature of the recruited foam cells. Moreover, we aimed to identify the epithelia-derived signals that drive macrophage infiltration and luminal translocation. Male C57BL/6J mice were implanted with slow-release testosterone and estradiol pellets (T+E2) and harvested the ventral prostates two weeks later for scRNA-seq analysis, or performed sham surgery. We identified Ear2+ and Cd72+ macrophages that were elevated in response to steroid hormone imbalance, whereas a Mrc1+ resident macrophage population did not change. In addition, an Spp1+ foam cell cluster was almost exclusively found in T+E2 mice. Further markers of foam cells were also identified, including Gpnmb and Trem2, and GPNMB was confirmed as a novel histological marker with immunohistochemistry. Foam cells were also shown to express known pathological factors Vegf, Tgfb1, Ccl6, Cxcl16 and Mmp12. Intriguingly, a screen for chemokines identified the upregulation of epithelial-derived Cxcl17, a known monocyte attractant, in T+E2 prostates suggesting that it might be responsible for the elevated macrophage number as well as their translocation to the lumen. Our study identified macrophage subsets that respond to steroid hormone imbalance as well as further confirmed a potential pathological role of luminal foam cells in the prostate. These results underscore a pathological role of the identified prostate foam cells and suggests CXCL17-mediated macrophage migration as a critical initiating event.

Keywords: benign prostatic hyperplasia; cytokines; foam cells; lower urinary tract symptoms.

Publication types

Preprint

Abstract

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