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口服避孕药和雌激素给药对绝经前后女性血浆降钙素的影响。

Effects of oral contraceptive and estrogen administration on plasma calcitonin in pre- and postmenopausal women.

作者信息

Hurley D L, Tiegs R D, Barta J, Laakso K, Heath H

机构信息

Department of Medicine, Mayo Clinic, Rochester, MN.

出版信息

J Bone Miner Res. 1989 Feb;4(1):89-95. doi: 10.1002/jbmr.5650040113.

DOI:10.1002/jbmr.5650040113
PMID:2718783
Abstract

Estrogen (E) therapy and administration of oral contraceptives (OC) reportedly increase plasma calcitonin (CT) concentrations in women, effects said to mediate in part the beneficial actions of E on bone. To further examine this theory, we tested the effects of three cycles of OC therapy in 12 young women, comparing them to 10 healthy women before and after three normal menstrual cycles. We also determined the effects of 3 months of E therapy (ethinyl estradiol, 20 micrograms/day, 25 of 30 days) in 14 healthy postmenopausal women, using a crossover design (studied after 3 months with and 3 months without E). We determined CT by radioimmunoassay (antiserum G-1701) in whole plasma (iCT) and silica cartridge extracts of plasma (exCT) after overnight fasting, after calcium (Ca) infusion (2 mg Ca/kg over 5 minutes), and during a normal day at 0800, 1200, 1700, and 2000 h. In no control study was there a significant diurnal change in iCT or exCT, and neither OC nor E therapy altered this. Similarly, OC administration did not affect basal CT levels or the normal iCT and exCT responses to Ca infusion. E therapy induced expected changes in serum Ca, phosphorus, and alkaline phosphatase and urinary Ca and cAMP excretion; basal and diurnal plasma exCT levels were decreased significantly, consonant with the decrement in serum Ca. E did not alter normal iCT and exCT responses to Ca infusion. Thus, administration of either OC or E has no stimulatory effect on CT secretion, which suggests that the beneficial actions of E on bone are not mediated through CT-induced inhibition of bone resorption.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

据报道,雌激素(E)疗法和口服避孕药(OC)的使用会增加女性血浆降钙素(CT)浓度,据说这种作用部分介导了E对骨骼的有益作用。为了进一步检验这一理论,我们测试了12名年轻女性三个周期OC疗法的效果,并将其与10名健康女性在三个正常月经周期前后进行比较。我们还采用交叉设计(在接受3个月E治疗和3个月无E治疗后进行研究),测定了14名健康绝经后女性接受3个月E治疗(炔雌醇,20微克/天,30天中的25天)的效果。我们通过放射免疫分析(抗血清G - 1701)测定空腹过夜后、钙输注(5分钟内输注2毫克钙/千克)后以及正常日8:00、12:00、17:00和20:00时全血血浆(iCT)和血浆硅胶柱提取物(exCT)中的CT。在任何对照研究中,iCT或exCT均无显著的昼夜变化,OC疗法和E疗法均未改变这一情况。同样,服用OC不影响基础CT水平或iCT和exCT对钙输注的正常反应。E疗法引起了血清钙、磷和碱性磷酸酶以及尿钙和环磷酸腺苷排泄的预期变化;基础和昼夜血浆exCT水平显著降低,与血清钙的降低一致。E并未改变iCT和exCT对钙输注的正常反应。因此,服用OC或E对CT分泌均无刺激作用,这表明E对骨骼的有益作用并非通过CT诱导的骨吸收抑制来介导。(摘要截取自250字)

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