Effect of Transdermal Estradiol and Oral Conjugated Estrogen on C-Reactive Protein in Retinoid-Placebo Trial in Healthy Women

A. Decensi, U. Omodei, C. Robertson, B. Bonanni, A. Guerrieri-Gonzaga, F. Ramazzotto, H. Johansson, S. Mora, M. Sandri, M. Cazzaniga, M. Franchi, S. Pecorelli
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引用次数: 128

Abstract

Background—The increase in C-reactive protein (CRP) during oral conjugated equine estrogen (CEE) may explain the initial excess of cardiovascular disease observed in clinical studies. Because the effect of transdermal estradiol (E2) on CRP is unclear, we compared CRP changes after 6 and 12 months of transdermal E2 and oral CEE in a randomized 2×2 retinoid-placebo trial. Methods and Results—A total of 189 postmenopausal women were randomized to 50 &mgr;g/d transdermal E2 and 100 mg BID of the retinoid fenretinide (n=45), 50 &mgr;g/d transdermal E2 and placebo (n=49), 0.625 mg/d oral CEE and 100 mg BID fenretinide (n=46), or 0.625 mg/d oral CEE and placebo (n=49) for 1 year. Sequential medroxyprogesterone acetate was added in each group. Relative to baseline, CRP increased by 10% (95% CI −9% to 33%) and by 48% (95% CI 22% to 78%) after 6 months of transdermal E2 and oral CEE, respectively. The corresponding figures at 12 months were 3% (95% CI −14% to 23%) for transdermal E2 and 64% (95% CI 38% to 96%) for oral CEE. Fenretinide did not change CRP levels at 6 and 12 months relative to placebo. Relative to oral CEE, the mean change in CRP after 12 months of transdermal E2 was −48% (95% CI −85% to −7%, P =0.012), whereas fenretinide was associated with a mean change of −1% (95% CI −34% to 40%, P =0.79) compared with placebo. Conclusions—In contrast to oral CEE, transdermal E2 does not elevate CRP levels up to 12 months of treatment. The implications for early risk of coronary heart disease require further studies.
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经皮雌二醇和口服结合雌激素对维生素a -安慰剂试验中健康女性c反应蛋白的影响
背景:口服结合马雌激素(CEE)期间c反应蛋白(CRP)的增加可能解释了临床研究中观察到的心血管疾病的初始过量。由于透皮雌二醇(E2)对CRP的影响尚不清楚,我们在一项随机2×2类视黄酮-安慰剂试验中比较了透皮E2和口服CEE在6个月和12个月后CRP的变化。方法与结果:共有189名绝经后妇女被随机分为50 g/d透皮E2和100 mg BID的类维生素a芬维甲酸组(n=45), 50 g/d透皮E2和安慰剂组(n=49), 0.625 mg/d口服CEE和100 mg BID的芬维甲酸组(n=46),或0.625 mg/d口服CEE和安慰剂组(n=49),为期1年。各组依次添加醋酸甲孕酮。相对于基线,经皮E2和口服CEE 6个月后,CRP分别增加了10% (95% CI - 9%至33%)和48% (95% CI 22%至78%)。12个月时的相应数据为透皮E2为3% (95% CI - 14% - 23%),口服CEE为64% (95% CI 38% - 96%)。与安慰剂相比,芬维啶在6个月和12个月时没有改变CRP水平。相对于口服CEE,经皮E2治疗12个月后CRP的平均变化为- 48% (95% CI - 85%至- 7%,P =0.012),而与安慰剂相比,芬维啶的平均变化为- 1% (95% CI - 34%至40%,P =0.79)。结论:与口服CEE相比,透皮E2在治疗12个月后不会升高CRP水平。对冠心病早期风险的影响需要进一步研究。
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