Oxytocin Receptor Antagonists As a Novel Pharmacological Agent for Reducing Smooth Muscle Tone in the Human Prostate

Overview

Journal Sci Rep

Specialty Science

Date 2021 Mar 19

PMID 33737570

Citations 3

Authors

Sophie N Lee

Jenna Kraska

Melissa Papargiris

Linda Teng

Birunthi Niranjan

Johanna Hammar

Andrew Ryan

Mark Frydenberg

Nathan Lawrentschuk

Ralf Middendorff

Stuart J Ellem

Michael Whittaker

Gail P Risbridger

Betty Exintaris

Affiliations

Soon will be listed here.

Abstract

Pharmacotherapies for the treatment of Benign Prostatic Hyperplasia (BPH) are targeted at reducing cellular proliferation (static component) or reducing smooth muscle tone (dynamic component), but response is unpredictable and many patients fail to respond. An impediment to identifying novel pharmacotherapies is the incomplete understanding of paracrine signalling. Oxytocin has been highlighted as a potential paracrine mediator of BPH. To better understand oxytocin signalling, we investigated the effects of exogenous oxytocin on both stromal cell proliferation, and inherent spontaneous prostate contractions using primary models derived from human prostate tissue. We show that the Oxytocin Receptor (OXTR) is widely expressed in the human prostate, and co-localises to contractile cells within the prostate stroma. Exogenous oxytocin did not modulate prostatic fibroblast proliferation, but did significantly (p < 0.05) upregulate the frequency of spontaneous contractions in prostate tissue, indicating a role in generating smooth muscle tone. Application of atosiban, an OXTR antagonist, significantly (p < 0.05) reduced spontaneous contractions. Individual tissue responsiveness to both exogenous oxytocin (R = 0.697, p < 0.01) and atosiban (R = 0.472, p < 0.05) was greater in tissue collected from older men. Overall, our data suggest that oxytocin is a key regulator of inherent spontaneous prostate contractions, and targeting of the OXTR and associated downstream signalling is an attractive prospect in the development of novel BPH pharmacotherapies.

Citing Articles

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