The oxytocin antagonist cligosiban reduces human prostate contractility: Implications for the treatment of benign prostatic hyperplasia

Author:

Bester Beatrix1ORCID,Koslowa Kristina1,Gronau Ann‐Catherine1,Mietens Andrea1,Nowell Cameron2,Whittaker Michael R.3,Pilatz Adrian4,Wagenlehner Florian4,Exintaris Betty2,Middendorff Ralf1

Affiliation:

1. Institute of Anatomy and Cell Biology Justus‐Liebig‐University Giessen Germany

2. Drug Discovery Biology Monash Institute of Pharmaceutical Sciences Melbourne Victoria Australia

3. Drug Discovery Disposition and Dynamics Monash Institute of Pharmaceutical Sciences Melbourne Victoria Australia

4. Department of Urology, Pediatric Urology, and Andrology Justus‐Liebig‐University Giessen Germany

Abstract

AbstractBackground and PurposeWith increasing life expectancy, benign prostatic hyperplasia (BPH) consequently affects more ageing men, illustrating the urgent need for advancements in BPH therapy. One emerging possibility may be the use of oxytocin antagonists to relax smooth muscle cells in the prostate, similar to the currently used (although often associated with side effects) α1‐adrenoceptor blockers.Experimental ApproachFor the first time we used live‐imaging, combined with a novel image analysis method, to investigate the multidirectional contractions of the human prostate and determine their changes in response to oxytocin and the oxytocin antagonists atosiban and cligosiban. Human prostate samples were obtained and compared from patients undergoing prostatectomy due to prostate cancer as well as from patients with transurethral resection of prostate tissue due to severe BPH.Key ResultsThe two cohorts of tissue samples showed spontaneous multidirectional contractions, which significantly increased after the addition of oxytocin. Different to atosiban, which showed ambiguous effects of short duration, only long‐acting cligosiban reliably prevented, as well as counteracted, any contractile oxytocin effect. Furthermore, cligosiban visibly reduced not only oxytocin‐induced contractions, but also showed intrinsic activity to relax prostatic tissue.Conclusion and implicationsThus, the oxytocin antagonist cligosiban could be an interesting candidate in the search for novel BPH treatment options.

Funder

Deutsche Forschungsgemeinschaft

Publisher

Wiley

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