Lack of influence of dyspareunia on the beneficial effect of intravaginal prasterone (dehydroepiandrosterone, DHEA) on sexual dysfunction in postmenopausal women

Fernand Labrie; David Archer; Céline Bouchard; Michel Fortier; Leonello Cusan; José-Luis Gomez; Ginette Girard; Mira Baron; Normand Ayotte; Michèle Moreau; Robert Dubé; Isabelle Côté; Claude Labrie; Lyne Lavoie; Lucy Gilbert; Céline Martel; John Balser

doi:10.1111/jsm.12517

Lack of influence of dyspareunia on the beneficial effect of intravaginal prasterone (dehydroepiandrosterone, DHEA) on sexual dysfunction in postmenopausal women

J Sex Med. 2014 Jul;11(7):1766-85. doi: 10.1111/jsm.12517. Epub 2014 Apr 28.

Authors

Fernand Labrie¹, David Archer, Céline Bouchard, Michel Fortier, Leonello Cusan, José-Luis Gomez, Ginette Girard, Mira Baron, Normand Ayotte, Michèle Moreau, Robert Dubé, Isabelle Côté, Claude Labrie, Lyne Lavoie, Lucy Gilbert, Céline Martel, John Balser

Affiliation

¹ EndoCeutics Inc., Quebec City, QC, Canada.

PMID: 24774442
DOI: 10.1111/jsm.12517

Abstract

Introduction: We have previously observed that intravaginal prasterone (dehydroepiandrosterone, DHEA) improved all domains of female sexual dysfunction (FSD).

Aim: Investigate the influence of moderate/severe pain at sexual activity (dyspareunia) (MSD) at baseline on FSD following prasterone administration.

Methods: The effect of daily administration of prasterone (0, 3.25 mg, 6.5 mg or 13 mg) for 12 weeks on FSD in 215 postmenopausal women with or without MSD at baseline was evaluated in a prospective, randomized, double-blind, and placebo-controlled phase III clinical trial.

Main outcome measures: Differences were examined on desire, arousal and orgasm.

Results: Comparable benefits were observed in women not having MSD (n = 56) vs. those having MSD (n = 159). The benefits over placebo in prasterone-treated women for desire, avoiding intimacy and vaginal dryness as well as for the total sexual domain of the MENQOL (Menopause Specific Quality of Life) questionnaire, ranged between 18.0% and 38.2% with P values of <0.05 or <0.01 except in one out of 12 subgroups. For the arousal/sensation, arousal/lubrication and summary score of the ASF (Abbreviated Sexual Function) questionnaire, in the MSD+ group, improvements of 64.2% (P = 0.01), 118% (P = 0.001) and 31.1% (P = 0.03) were observed over placebo, respectively, while similar differences (58.0%, 67.6% and 32.1%) did not reach statistical significance in the MSD- group having up to only 44 prasterone-treated women compared with 119 in the MSD+ group.

Conclusions: No MSD at baseline does not apparently affect the effects of intravaginal prasterone on sexual dysfunction. Knowing the absence of significant effects of estrogens on FSD, the present data suggest that vulvovaginal atrophy (VVA) and vulvovaginal sexual dysfunction (VVSD) are two different consequences of sex steroid deficiency at menopause which can respond independently. In addition, the present data seriously question the justification of pain being part of FSD as well as the separation of FSD into separate domains.

Keywords: Androgens; Dehydroepiandrosterone (DHEA); Female Sexual Dysfunction; Intracrinology; Low Arousal; Low Desire; Nerve fibers; Vagina.

Publication types

Clinical Trial, Phase III
Comparative Study
Multicenter Study
Randomized Controlled Trial

MeSH terms

Administration, Intravaginal
Adult
Aged
Androgens / administration & dosage*
Arousal / drug effects
Dehydroepiandrosterone / administration & dosage*
Double-Blind Method
Dyspareunia / complications*
Estrogens / therapeutic use
Female
Humans
Menopause
Middle Aged
Nerve Fibers / drug effects
Orgasm / drug effects
Postmenopause / drug effects
Prospective Studies
Quality of Life
Sexual Behavior / drug effects
Sexual Dysfunctions, Psychological / drug therapy*
Suppositories
Surveys and Questionnaires
Vagina / innervation
Vaginal Diseases / drug therapy

Substances

Androgens
Estrogens
Suppositories
Dehydroepiandrosterone