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Review
. 2015 Jul;22(7):786-96.
doi: 10.1097/GME.0000000000000365.

Effects of ospemifene on the female reproductive and urinary tracts: translation from preclinical models into clinical evidence

Affiliations
Review

Effects of ospemifene on the female reproductive and urinary tracts: translation from preclinical models into clinical evidence

David F Archer et al. Menopause. 2015 Jul.

Abstract

Objective: Treatment of menopausal symptoms by compounds with tissue-selective estrogen agonist/antagonist effects, often called selective estrogen receptor modulators, has been researched as an alternative to the use of estrogen therapy. These structurally diverse molecules elicit tissue-dependent responses in hormone-responsive tissues and organs, exhibiting variations in estrogenic activity in preclinical models of postmenopausal reproductive tissues that may improve postmenopausal women's health (eg, prevention and treatment of breast cancer, osteoporosis, and vulvar and vaginal atrophy).

Methods: This literature review investigates whether preclinical data predicted the clinical effects of ospemifene on female reproductive and urinary tract tissues and compares these findings with the specific vaginal effects of other estrogen receptor agonists/antagonists (tamoxifen, raloxifene, and bazedoxifene) in preclinical and clinical studies. Lasofoxifene, although not currently available, is included because of its unique effects on vaginal tissue.

Results: The response of endometrial and vaginal tissues to estrogen receptor agonists/antagonists can be differentiated using transvaginal ultrasound, endometrial histopathology, cytologic examination of vaginal smears, assessment of physical changes in the vagina, and relief of symptoms associated with vulvar and vaginal atrophy (such as dyspareunia).

Conclusions: Available evidence indicates that ospemifene has unique effects on tissue, leading to a favorable long-term profile for the relief of vulvar and vaginal atrophy compared with other estrogen receptor agonists/antagonists (eg, tamoxifen, raloxifene, and bazedoxifene) with no short-term concerns about endometrial safety (based on endometrial hyperplasia, carcinoma, endometrial spotting, and endometrial bleeding).

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Conflict of interest statement

Financial disclosure/conflicts of interest: D.F.A. serves as consultant to Shionogi Inc, Agile Therapeutics, AbbVie, Bayer Healthcare, CHEMO, Endoceutics, HRA Pharma, and TEVA, and serves at the speakers bureau for Pfizer, Shionogi Inc, Agile Therapeutics, and Merck. B.R.C. serves at the speakers bureau for Shionogi Inc, Pfizer, and Noven Pharmaceuticals Inc, and has received grants/research support (funds to the University of Texas) from AbbVie. In the past 12 months, J.V.P. has served as consultant (fees to the University of Virginia) to Pfizer Inc, Noven Pharmaceuticals Inc, Novo Nordisk, DepoMed, Shionogi, and TherapeuticsMD; has received grants/research support (fees to the University of Virginia) from DepoMed, Bionova, TherapeuticsMD, and Endoceutics; has received travel funds from Pfizer Inc, Noven Pharmaceuticals Inc, DepoMed, Novo Nordisk, Endoceutics, and Shionogi; and has received editorial writing support from Pfizer Inc, Shionogi, and Noven Pharmaceuticals Inc. H.S.T. has served as consultant to Pfizer, AbbVie, Medistem, and Ovascience. G.D.C. has served as consultant to pharmaceutical companies including, but not limited to, Shionogi Inc and TherapeuticsMD. G.D.C. is a former employee of Wyeth and Pfizer.

Figures

FIG.
FIG.
Estrogen receptor agonist/antagonist mechanism of action via binding to the ER-α or ER-β receptor and eliciting specific nuclear coactivators and corepressors. ERAA, estrogen receptor agonist/antagonist; ER, estrogen receptor; CoA, coenzyme A.

References

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