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Oral absorption and presystemic first-pass effect of chlorpheniramine in rabbits
Authors:Shiew-Mei Huang  Yih-Chain Huang  Win L Chiou
Institution:(1) Department of Pharmacy, College of Pharmacy, University of Illinois at the Medical Center, 60612 Chicago, Illinois;(2) Present address: Drug Metabolism, Ortho Pharmaceutical Corporation, 08869 Raritan, New Jersey;(3) Present address: College of Pharmacy, Rutgers-The State University, 08854 Piscataway, New Jersey
Abstract:The oral absolute bioavailabilities of chloropheniramine (CPM) in four rabbits (New Zealand White, male, mean wt. 3.71 kg), averaged 0.06±0.03, 0.11±0.08, and 0.09±0.01 following a 3, 10.5, and 21 mg/kg dose, respectively. The individual bioavailability data and the AUCof one of the demethylated metabolites, desdimethyl CPM (DDCPM) obtained following different doses suggested the existence of saturable presystemic elimination. Two rabbits received an additional 10.5 mg/kg dose of CPM through portal vein infusion. Based on the oral, intraportal vein and i.v. studies, the mean extraction ratios of gut and the liver calculated for these two rabbits averaged 0.58 and 0.76, respectively. The latter value agreed well with the estimated hepatic extraction ratio from the in vitro liver homogenate study (0.89) or from the i.v. studies (0.83). The extensive prehepatic first-pass effect observed in the present study was consistent with similar findings in humans and dogs.
Keywords:pharmacokinetics  chlorpheniramine  first-pass effect  bioavailability  gut metabolism
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