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Journal of Clinical Endocrinology & Metabolism, doi:10.1210/jc.2004-0727
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The Journal of Clinical Endocrinology & Metabolism Vol. 90, No. 1 142-146
Copyright © 2005 by The Endocrine Society

Levels of Serum C-Reactive Protein during Oral and Transdermal Estradiol in Postmenopausal Women with and without a History of Intrahepatic Cholestasis of Pregnancy

A. Ropponen, K. Aittomäki, M. J. Tikkanen and O. Ylikorkala

Departments of Obstetrics and Gynecology (A.R., O.Y.), Medical Genetics (K.A.), and Medicine (M.J.T.), Helsinki University Central Hospital, FIN-00029, Helsinki, Finland

Address all correspondence and requests for reprints to: Olavi Ylikorkala, Professor, Department of Obstetrics and Gynecology, Helsinki University Central Hospital, P.O. Box 140, FIN-00029 HUS, Helsinki, Finland. E-mail: olavi.ylikorkala{at}hus.fi.

Liver dysfunction may affect the production and release of C-reactive protein (CRP). We designed a double-blind prospective crossover study involving 40 postmenopausal women with or without a history of intrahepatic cholestasis of pregnancy (ICP), where we compared the basal levels of CRP and their responses to increasing doses of oral and transdermal estradiol (E2), followed by addition of oral medroxyprogesterone acetate (MPA). Serum samples collected at baseline, on the last day of each E2 period, and on the last day of the E2 + MPA combination were assayed for CRP, estrogens, and liver enzymes. There was no difference in basal CRP between the study groups. Both regimens (oral and transdermal E2) were accompanied by significant rises in estrone and E2 concentrations; the former were 16 times higher during the oral than during the transdermal regimen. Oral E2 elevated CRP dose dependently, and this response was unaffected by a history of ICP or the use of MPA. The activities of liver transaminases varied but were in normal ranges during E2 use, in women with and without a history of ICP. In conclusion, the synthesis of CRP is not affected by a history of ICP. It is readily and dose dependently stimulated by oral but not by transdermal E2 in as soon as 2 wk.




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