Urethral luminal epithelia are castration-insensitive cells of the proximal prostate

Diya B. Joseph PhD, Gervaise H. Henry MS, Alicia Malewska MS, Nida S. Iqbal PhD, Hannah M. Ruetten, Anne E. Turco, Lisa L. Abler PhD, Simran K. Sandhu, Mark T. Cadena, Venkat S. Malladi MS, Jeffrey C. Reese MD, Ryan J. Mauck MD, Jeffrey C. Gahan MD, Ryan C. Hutchinson MD, Claus G. Roehrborn MD, Linda A. Baker MD, Chad M. Vezina PhD, Douglas W. Strand PhD

Abstract

Background: Castration‐insensitive epithelial progenitors capable of regenerating the prostate have been proposed to be concentrated in the proximal region based on facultative assays. Functional characterization of prostate epithelial populations isolated with individual cell surface markers has failed to provide a consensus on the anatomical and transcriptional identity of proximal prostate progenitors. Methods: Here, we use single‐cell RNA sequencing to obtain a complete transcriptomic profile of all epithelial cells in the mouse prostate and urethra to objectively identify cellular subtypes. Pan‐transcriptomic comparison to human prostate cell types identified a mouse equivalent of human urethral luminal cells, which highly expressed putative prostate progenitor markers. Validation of the urethral luminal cell cluster was performed using immunostaining and flow cytometry. Results: Our data reveal that previously identified facultative progenitors marked by Trop2, Sca‐1, KRT4, and PSCA are actually luminal epithelial cells of the urethra that extend into the proximal region of the prostate, and are resistant to castration‐induced androgen deprivation. Mouse urethral luminal cells were identified to be the equivalent of previously identified human club and hillock cells that similarly extend into proximal prostate ducts. Benign prostatic hyperplasia (BPH) has long been considered an “embryonic reawakening,” but the cellular origin of the hyperplastic growth concentrated in the periurethral region is unclear. We demonstrate an increase in urethral luminal cells within glandular nodules from BPH patients. Urethral luminal cells are further increased in patients treated with a 5‐α reductase inhibitor. Conclusions: Our data demonstrate that cells of the proximal prostate that express putative progenitor markers, and are enriched by castration in the proximal prostate, are urethral luminal cells and that these cells may play an important role in the etiology of human BPH.

Datasets

1. Urethral luminal epithelia are castration-insensitive cells of the proximal prostate - All Human Cells
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D17PrPzF_Via3813 cells
BPH342PrF_Via3596 cells
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D27PrTzF_Via3325 cells
BPH340PrGF_Via3219 cells
D17PrTzF_Via3143 cells
BPH327PrGF_Via3109 cells
D35PrTzF_Via2819 cells
D35PrPzF_Via2234 cells
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Urethral luminal epithelia are castration-insensitive cells of the proximal prostate

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Source data

https://cellxgene.cziscience.com/collections/fbc5881f-1ee3-4ffe-8095-35e15e1a08fc

Alias names

PMID32497356, PMC7339731

Cite this study

Joseph, D.B., Henry, G.H., Malewska, A., Iqbal, N.S., Ruetten, H.M., Turco, A.E., Abler, L.L., Sandhu, S.K., Cadena, M.T., Malladi, V.S. and Reese, J.C., 2020. Urethral luminal epithelia are castration‐insensitive cells of the proximal prostate. The Prostate, 80(11), pp.872-884. https://doi.org/10.1002/pros.24020