Disclosure: The preparation of this review was not supported by any external funding.
Conflicts of interest: Young-A Heo is salaried employees of Adis International Ltd/Springer Nature, is responsible for the article content and declares no relevant conflicts of interest.
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Abstract
Vulvovaginal atrophy (VVA) is a progressive condition commonly seen in postmenopausal women. The
cessation of ovarian estrogen secretion and a fall in serum levels of dehydroepiandrosterone (DHEA), the remaining
source of estrogens and androgens, are thought to promote the development of VVA in
this population. Intravaginal prasterone (Intrarosa®) is a synthetic form of DHEA indicated for the
treatment of VVA in postmenopausal women presenting with moderate to severe
symptoms in the EU; prasterone is also approved in the USA for the treatment of
dyspareunia due to menopause. Approval for the treatment of VVA was based on
the results of the phase III ERC-231 and -238 trials in which intravaginal prasterone
6.5 mg/day significantly improved the signs and symptoms of VVA (as assessed by
the percentage of parabasal and superficial cells, vaginal pH and the severity
of dyspareunia) compared with placebo. The beneficial effects of prasterone
were also evident during 52 weeks’ treatment in the phase III ERC-230 safety trial.
Prasterone was generally well tolerated, with the most common
treatment-emergent adverse event being application site discharge. During 52
weeks of treatment with prasterone, changes in serum concentrations of estrogenic and androgenic metabolites of DHEA increased from baseline but remained within the normal postmenopausal ranges. Thus, intravaginal prasterone is an effective
and generally well-tolerated option for the treatment of VVA in postmenopausal
women.