AUTHOR=Esquivel-Franco Diana Carolina , de Boer Sietse F. , Waldinger Marcel , Olivier Berend , Olivier Jocelien D. A. 

TITLE=Pharmacological Studies on the Role of 5-HT1A Receptors in Male Sexual Behavior of Wildtype and Serotonin Transporter Knockout Rats

JOURNAL=Frontiers in Behavioral Neuroscience

VOLUME=14

YEAR=2020

URL=https://www.frontiersin.org/journals/behavioral-neuroscience/articles/10.3389/fnbeh.2020.00040

DOI=10.3389/fnbeh.2020.00040

ISSN=1662-5153

ABSTRACT=<p>Brain serotonin (5-HT) neurotransmission plays an important role in male sexual behavior and it is well established that activating 5-HT<sub>1</sub><sub>A</sub> receptors in rats facilitate ejaculatory behavior. However, the relative contribution of 5-HT<sub>1</sub><sub>A</sub> somatodendritic autoreceptors and heteroreceptors in this pro-sexual behavior is unclear. Moreover, it is unclear whether the contribution of somatodendritic 5-HT<sub>1</sub><sub>A</sub> autoreceptors and postsynaptic 5-HT<sub>1</sub><sub>A</sub> heteroreceptors alter when extracellular 5-HT levels are chronically increased. Serotonin transporter knockout (SERT<sup>–/–</sup>) rats exhibit enhanced extracellular 5-HT levels and desensitized 5-HT<sub>1</sub><sub>A</sub> receptors. These rats model neurochemical changes underlying chronic SSRI-induced sexual dysfunction. We want to determine the role of presynaptic versus postsynaptic 5-HT<sub>1</sub><sub>A</sub> receptors in the pro-sexual effects of 5-HT<sub>1</sub><sub>A</sub> receptor agonists in SERT<sup>+/+</sup> and in SERT<sup>–/–</sup> rats. Therefore, acute effects of the biased 5-HT<sub>1</sub><sub>A</sub> receptor agonists F-13714, a preferential 5-HT<sub>1</sub><sub>A</sub> autoreceptor agonist, or F-15599, a preferential 5-HT<sub>1</sub><sub>A</sub> heteroreceptor agonist, and S15535 a mixed 5-HT<sub>1</sub><sub>A</sub> autoreceptor agonist/heteroreceptor antagonist, on male sexual behavior were assessed. A clear and stable genotype effect was found after training where SERT<sup>+/+</sup> performed sexual behavior at a higher level than SERT<sup>–/–</sup> rats. Both F-15599 and F-13714 induced pro-sexual activity in SERT<sup>+/+</sup> and SERT<sup>–/–</sup> animals. Compared to SERT<sup>+/+</sup>, the F13714-dose-response curve in SERT<sup>–/–</sup> rats was shifted to the right. SERT<sup>+/+</sup> and SERT<sup>–/–</sup> rats responded similar to F15599. Within both SERT<sup>+/+</sup> and SERT<sup>–/–</sup> rats the potency of F-13714 was much stronger compared to F-15599. S15535 had no effect on sexual behavior in either genotype. In SERT<sup>+/+</sup> and SERT<sup>–/–</sup> rats that were selected on comparable low sexual activity (SERT<sup>+/+</sup> 3 or less ejaculations and SERT<sup>–/–</sup> 5 or less ejaculations in 10 weeks) S15535 also did not influence sexual behavior. The two biased compounds with differential effects on 5-HT<sub>1</sub><sub>A</sub> auto- and hetero-receptors, exerted pro-sexual activity in both SERT<sup>+/+</sup> and SERT<sup>–/–</sup> rats. Applying these specific pharmacological tools has not solved whether pre- or post-synaptic 5-HT<sub>1</sub><sub>A</sub> receptors are involved in pro-sexual activity. Moreover, the inactivity of S15535 in male sexual behavior in either genotype was unexpected. The question is whether the <italic>in vivo</italic> pharmacological profile of the different 5-HT<sub>1</sub><sub>A</sub> receptor ligands used, is sufficient to differentiate pre- and/or post-synaptic 5-HT<sub>1</sub><sub>A</sub> receptor contributions in male rat sexual behavior.</p>