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Effects of Kisspeptin Administration in Women With Hypoactive Sexual Desire Disorder

吻素 性欲低下障碍 遗产管理(遗嘱认证法) 心理学 性欲 医学 内分泌学 性别研究 人类性学 社会学 政治学 激素 法学
作者
Layla Thurston,Tia Hunjan,Natalie Ertl,Matthew B. Wall,Edouard Mills,Sofiya Suladze,Bjial Patel,Emma Alexander,Beatrice Muzi,Paul Bassett,Eugenii A. Rabiner,Paul Bech,David Goldmeier,Ali Abbara,Alexander Comninos,Waljit S. Dhillo
出处
期刊:JAMA network open [American Medical Association]
卷期号:5 (10): e2236131-e2236131 被引量:17
标识
DOI:10.1001/jamanetworkopen.2022.36131
摘要

Importance Despite being the most common female sexual health complaint worldwide, current treatment options for hypoactive sexual desire disorder (HSDD) are limited in their safety and effectiveness. The hormone kisspeptin is a key endogenous activator of the reproductive hormonal axis with additional emerging roles in sexual and emotional behavior; however, its effects in women with HSDD are unknown. Objective To test the hypothesis that kisspeptin enhances sexual and attraction brain processing in women with HSDD. Design, Setting, and Participants This randomized clinical trial was double-masked and placebo controlled with a 2-way crossover. The trial was conducted in a university research setting in the UK from October 2020 to April 2021. Eligible participants were premenopausal women with HSDD. Functional neuroimaging, psychometric, and hormonal analyses were employed to investigate the effects of kisspeptin administration on brain processing, in response to erotic stimuli (erotic videos) and facial attraction (face images of varying attractiveness). Data were analyzed from May to December 2021. Interventions A 75-minute intravenous infusion of kisspeptin-54 (1 nmol/kg/h) vs equivalent-rate placebo infusion. Main Outcomes and Measures Blood oxygen level–dependent responses across the whole brain and regions of interest during kisspeptin vs placebo administration in response to erotic and facial attraction stimuli. Results Of the 40 participants who were randomized, 32 women completed both kisspeptin and placebo visits, with a mean (SE) age of 29.2 (1.2) years. Kisspeptin administration resulted in modulations in sexual and facial attraction brain processing (deactivation of the left inferior frontal gyrus: Z max, 3.76; P = .01; activation of the right postcentral and supramarginal gyrus: Z max, 3.73; P < .001; deactivation of the right temporoparietal junction: Z max 4.08; P = .02). Furthermore, positive correlations were observed between kisspeptin-enhanced hippocampal activity in response to erotic videos, and baseline distress relating to sexual function ( r = 0.469; P = .007). Kisspeptin’s enhancement of posterior cingulate cortex activity in response to attractive male faces also correlated with reduced sexual aversion, providing additional functional significance ( r = 0.476, P = .005). Kisspeptin was well-tolerated with no reported adverse effects. Conclusions and Relevance These findings lay the foundations for clinical applications for kisspeptin in women with HSDD. Trial Registration ISRCTN trial registry identifier: ISRCTN17271094
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