Title of article
Progesterone abolishes estrogen and/or atorvastatin endothelium dependent vasodilatory effects
Author/Authors
André Arpad Faludi، نويسنده , , José Mendes Aldrighi، نويسنده , , Marcelo Chiara Bertolami، نويسنده , , Mohamed H. Saleh، نويسنده , , Renata Alves Silva، نويسنده , , Yara Nakamura، نويسنده , , Isabela R.O. Pereira، نويسنده , , Dulcineia Saes Parra Abdalla، نويسنده , , José Antonio Franchini Ramires، نويسنده , , Jose Eduardo M.R. Sousa، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 2004
Pages
8
From page
89
To page
96
Abstract
This double blind randomized placebo controlled study assessed the effects of atorvastatin, estradiol and norethisterone, isolated and in combination, on the lipid profile and on vascular reactivity, in post-menopausal women with hypercholesterolemia and arterial hypertension. Ninety-four women aged 50–65 were selected. All have received dietary counseling (4 weeks), placebo (4 weeks), and drug therapy (12 weeks): 17-β estradiol 2mg/day (E) (n = 17); E + norethisterone acetate 1 mg/day (P) (n = 18); Atorvastatin 10 mg/day (A) (n = 20); E + A (n = 21) and E + P + A (n = 18). All treatment modalities have significantly reduced total cholesterol (TC) (E = 8.8%, E + P = 10.1%, A = 27.9%, A + E = 29.4% and E + P + A = 35.7%) and LDL-cholesterol (LDL-c) levels (E + P + A = 46.6%, E + A = 45.9%, A = 40.2%, E = 20.3%, and E + P = 12.1%). As concerns HDL-cholesterol (HDL-c), Groups E and E + A had increases of 15.5% and 13.1%, respectively. The addition of a progesterone compound reduced its concentration (Group E + P = −9.1%, and Group E + P + A = −9.5%). By random, approximately half of the patients in each group were designated to the endothelial function evaluation (brachial artery ultrasound). We observed that in Group A (n = 10), in Group E (n = 10) and with the association (Group E + A) (n = 7), there was a significant increase in the flow-mediated vasodilatation as compared to basal measurements. The addition of a progestin has annulled these benefits. Conclusions: Atorvastatin has promoted more beneficial effects on TC and LDL-c, whereas estradiol was responsible for an increase in HDL-c. The addition of a progesterone derivative abolished these benefits. Atorvastatin, estradiol or both together improved endothelial function, an effect suppressed by the addition of norethisterone.
Keywords
hormonal replacement therapy , endothelial function , atorvastatin , hypertension , Menopause , Hypercholesterolemia
Journal title
Atherosclerosis
Serial Year
2004
Journal title
Atherosclerosis
Record number
631464
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