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Thirty-day rat toxicity study reveals reversible liver toxicity of mifepristone (RU486) and metapristone
Authors:Yingying Xiao  Yewei Zhu  Suhong Yu  Cuicui Yan  Rodney J Y Ho  Jian Liu
Institution:1. Cancer Metastasis Alert and Prevention Center, and Pharmaceutical Photocatalysis of State Key Laboratory of Photocatalysis on Energy and Environment, College of Chemistry, Fuzhou University, Fuzhou, China,;2. Department of Pharmaceutics, University of Washington, Seattle, WA, USA, and
Abstract:Objective: Mifepristone (RU486) is an oral first-line contraceptive used by hundreds of millions of women, and recently it was tested for anticancer activity in both genders worldwide. We are developing metapristone (the N-monodemethyl RU486) as a potential metastasis chemopreventive. The present acute and 30-d subacute toxicity study aimed at examining and compared in parallel the potential toxicity of the two drugs.

Methods: The single-dose acute toxicity and 30-d subacute toxicity studies were conducted in mice and rats, respectively, by gavaging metapristone or mifepristone at various doses. Blood samples and organs were collected for blood chemistry, hematology and histology analyses.

Results: Oral mifepristone (3000?mg/kg) caused 30% and 40% death in female and male mice, respectively, within 15 h post-dosing. In comparison, the same dose of metapristone produced 30% acute death in males only. Thirty-day oral administration of the two drugs to rats (12.5, 50 and 200?mg/kg/day) caused reversible hepatotoxicity that only occurred at 200?mg/kg/day group, evidenced by the elevated liver enzyme activity and liver organ weight.

Conclusion: The present study, for the first time, reveals reversible hepatotoxicity in rats caused by the 30-d consecutive administration at the high dose, and warns the potential hepatotoxicity caused by long-term administrations of high doses of mifepristone or metapristone in clinical trials but not by the acute single abortion doses.
Keywords:Acute toxicity  liver toxicity  metapristone  mifepristone  subacute toxicity
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