Characteristics of α1‐adrenoceptor antagonists‐induced ejaculatory dysfunction on spontaneous seminal emission in rats

Author:

Yoshizumi Masaru1ORCID,Ise Shin‐nosuke1,Yonezawa Akihiko2,Watanabe Chizuko1,Sakurada Shinobu1,Mizoguchi Hirokazu1

Affiliation:

1. Division of Physiology and Anatomy, Faculty of Pharmaceutical Sciences Tohoku Medical and Pharmaceutical University Sendai Japan

2. Division of Pharmaceutical Center, Faculty of Pharmaceutical Sciences Tohoku Medical and Pharmaceutical University Sendai Japan

Abstract

AbstractAlthough α1‐adrenoceptor (α1‐AR) antagonists used to treat benign prostatic hyperplasia can cause ejaculation disorders, the aetiology of this adverse event is still controversial. Therefore, we investigated the effects of antagonists with different affinities for α1‐AR subtypes on ejaculatory function and their mechanisms of action in normal rats. In the spontaneous seminal emission (SSE) test, systemically administered prazosin, terazosin, tamsulosin and naftopidil decreased the weight of ejaculated seminal material in a dose‐dependent manner; the potency order was as follows: tamsulosin > terazosin > prazosin > naftopidil. The selective α1D‐AR antagonist BMY7378 had no effect on SSE. Intrathecal tamsulosin and naftopidil did not inhibit SSE. Tamsulosin, the most potent, was ineffective as a single dose and significantly increased seminal vesicle fluid in rats treated for 2 weeks but did not significantly change retrograde ejaculation. These results indicated that the difference in inhibitory potency of the five α1‐AR antagonists against SSE was due to the involvement of α1A‐AR subtypes. Our results further suggested that α1‐AR antagonist‐induced ejaculatory dysfunction at the peripheral level was mainly due to the loss of seminal emission, although some retrograde ejaculation may also be involved.

Funder

Japan Society for the Promotion of Science

Publisher

Wiley

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