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一项关于美托咪定和阿替美唑在泌乳奶牛体内的药代动力学研究,包括一些相关的临床效果。

A pharmacokinetic study including some relevant clinical effect of medetomidine and atipamezole in lactating dairy cows.

作者信息

Ranheim B, Arnemo J M, Ryeng K A, Søli N E, Horsberg T E

机构信息

Department of Pharmacology, Microbiology and Food Hygiene, The Norwegian School of Veterinary Science, Oslo.

出版信息

J Vet Pharmacol Ther. 1999 Dec;22(6):368-73. doi: 10.1046/j.1365-2885.1999.00231.x.

DOI:10.1046/j.1365-2885.1999.00231.x
PMID:10651465
Abstract

Medetomidine is the most potent and selective alpha2-agonist used in veterinary medicine and its effects can be antagonized by the alpha2-antagonist atipamezole. The pharmacokinetics of medetomidine and atipamezole were studied in a cross-over trial in eight lactating dairy cows. The animals were injected intravenously (i.v.) with medetomidine (40 microg/kg) followed by atipamezole i.v. (200 microg/kg) or saline i.v. after 60 min. Drug concentrations in plasma were measured by HPLC. After the injection of atipamezole, the concentration of medetomidine in plasma increased slightly, the mean increment being 2.7 ng/mL and the mean duration 12.1 min. However, atipamezole did not alter the pharmacokinetics of medetomidine. It is likely that the increase in medetomidine concentration is caused by displacement of medetomidine by atipamezole in highly perfused tissues. The volume of distribution at steady state (Vss) for medetomidine followed by saline and medetomidine followed by atipamezole was 1.21 and 1.32 L/kg, respectively, whereas the total clearance (Cl) values were 24.2 and 25.8 mL/min x kg. Vss and Cl values for atipamezole were 1.77 mL/kg and 48.1 mL/min x kg, respectively. Clinically, medetomidine significantly reduced heart rate and increased rectal temperature for 45 min. Atipamezole reversed the sedative effects of medetomidine. However, all the animals, except one, relapsed into sedation at an average of 80 min after injection of the antagonist.

摘要

美托咪定是兽医学中使用的效力最强且选择性最高的α2-激动剂,其作用可被α2-拮抗剂阿替美唑所拮抗。在一项交叉试验中,对8头泌乳奶牛的美托咪定和阿替美唑的药代动力学进行了研究。给这些动物静脉注射(i.v.)美托咪定(40微克/千克),60分钟后再静脉注射阿替美唑(200微克/千克)或生理盐水。通过高效液相色谱法(HPLC)测定血浆中的药物浓度。注射阿替美唑后,血浆中美托咪定的浓度略有升高,平均增量为2.7纳克/毫升,平均持续时间为12.1分钟。然而,阿替美唑并未改变美托咪定的药代动力学。美托咪定浓度升高可能是由于在灌注良好的组织中,阿替美唑将美托咪定置换出来所致。美托咪定后接生理盐水以及美托咪定后接阿替美唑时,美托咪定的稳态分布容积(Vss)分别为1.21和1.32升/千克,而总清除率(Cl)值分别为24.2和25.8毫升/分钟×千克。阿替美唑的Vss和Cl值分别为1.77毫升/千克和48.1毫升/分钟×千克。临床上,美托咪定可使心率显著降低,并使直肠温度升高45分钟。阿替美唑可逆转美托咪定的镇静作用。然而,除1只动物外,所有动物在注射拮抗剂后平均80分钟时又重新陷入镇静状态。

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