Literature DB >> 619226

Heparin resistance and decreased hepatic triglyceride hydrolase release during long-term estrogen-progestin treatment.

B W Glad, D E Wilson, D B Cook, P K Working, M E Adler.   

Abstract

These studies were undertaken to define the mechanism for the depression of post-heparin triglyceride hydrolase activity in women treated with estrogen-progestin oral contraceptives. Six treated and six control women were studied. Total, protamine-inhibited, and protamine-resistant triglyceride hydrolase activities were measured after six different intravenous doses of heparin in each subject in order to determine the dose-response relationships for lipase release. As has been reported during short-term treatment with estrogens, long-term treatment with oral contraceptive agents is accompanied by selective depression of protamine-resistant (hepatic) lipase activity. This depression can be partly reversed by the administration of large heparin doses, but maximally releasing heparin does fail to restore postheparin protamine-resistant activity to control values. These data are compatible with the idea that the releasable pool of hepatic triglyceride hydrolase activity is diminished in women who receive oral contraceptive agents and that the pharmacokinetics of its release are altered in such a way that only relatively high concentrations of heparin displace the enzyme from this pool.

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Year:  1978        PMID: 619226     DOI: 10.1016/0026-0495(78)90123-3

Source DB:  PubMed          Journal:  Metabolism        ISSN: 0026-0495            Impact factor:   8.694


  1 in total

1.  Prednisone treatment alters the serum amylase and lipase activities in normal dogs without causing pancreatitis.

Authors:  C Fittschen; J E Bellamy
Journal:  Can J Comp Med       Date:  1984-04
  1 in total

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