Abstract

ABSTRACT Introduction Those suffering with vaginal dryness, whether experienced once or chronically, frequently experience painful and unpleasurable sexual experiences and diminished self-esteem as a result. Although the physiology of vaginal transudate production is long established, no pharmacological treatment other than estrogen has shown promise in attenuating vaginal dryness. Previously, our lab has shown that methamphetamine (meth) induced vaginal lubrication in adult women and anesthetized rats. The production of these vaginal secretions was shown to be dose-, as well as nitric oxide-dependent. As the secretion of vaginal lubrication is immensely dependent on local hemodynamics and the resulting increased blood flow to the genital tissues, determining meth-induced alterations in blood flow to these tissues is paramount. Objective The purpose of the current study is to determine if increased vaginal blood flow correlates with increased vaginal lubrication in response to meth, and to determine if alterations in this blood flow are nitric oxide-dependent. Methods Adult female Wistar rats were implanted with chronic indwelling jugular catheters and allowed at least one week to recover from surgery. Rats anesthetized with isoflurane gas were intravenously infused with meth (0.06-0.96 mg/kg) or saline via the implanted catheter. Vaginal blood flow, measured using a Periflux System 5000 and a small laser probe inserted 5-10 mm into the vaginal canal, was continuously recorded before and for at least twenty minutes following drug administration. After establishing meth-induced alterations in vaginal blood flow, pre-treatment with L-NG-Nitro arginine methyl ester (L-NAME), a non-specific nitric oxide synthase inhibitor, followed by meth administration following the same procedure for measuring blood flow allowed us to determine the contribution of nitric oxide to the observed changes in blood flow. Results Preliminary findings show that an IV infusion of meth induces an immediate increase in vaginal blood flow, followed by decreased blood flow due to vasoconstriction via increased sympathetic tone. We anticipate inhibition of nitric oxide production will reduce the increase in blood flow immediately after meth administration since this decreased vaginal lubrication in response to the same treatment. Conclusions These findings provide insight into the meth-induced vaginal lubrication we have previously reported, and that meth, whose sympathomimetic action traditionally induces vasoconstriction, produces increased blood flow in vaginal tissues, which is likely the driving force for the increased transudate produced. This advancement is critical for uncovering a mechanism that may serve as the optimal pharmacological target to treat vaginal dryness. Disclosure Any of the authors act as a consultant, employee or shareholder of an industry for: Embera NeuroTherapeutics & JanOne

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