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泛昔洛韦及其活性代谢产物喷昔洛韦在亚洲象幼象(印度象)体内的药代动力学估算。

Estimates of the pharmacokinetics of famciclovir and its active metabolite penciclovir in young Asian elephants (Elephas maximus).

作者信息

Brock A Paige, Isaza Ramiro, Hunter Robert P, Richman Laura K, Montali Richard J, Schmitt Dennis L, Koch David E, Lindsay William A

机构信息

Department of Small Animal Clinical Sciences, College of Veterinary Medicine, University of Florida, Gainesville, FL 32608, USA.

出版信息

Am J Vet Res. 2012 Dec;73(12):1996-2000. doi: 10.2460/ajvr.73.12.1996.

Abstract

OBJECTIVE

To determine plasma pharmacokinetics of penciclovir following oral and rectal administration of famciclovir to young Asian elephants (Elephas maximus).

ANIMALS

6 healthy Asian elephants (5 females and 1 male), 4.5 to 9 years old and weighing 1,646 to 2,438 kg.

PROCEDURES

Famciclovir was administered orally or rectally in accordance with an incomplete crossover design. Three treatment groups, each comprising 4 elephants, received single doses of famciclovir (5 mg/kg, PO, or 5 or 15 mg/kg, rectally); there was a minimum 12-week washout period between subsequent famciclovir administrations. Serial blood samples were collected after each administration. Samples were analyzed for famciclovir and penciclovir with a validated liquid chromatography-mass spectroscopy assay.

RESULTS

Famciclovir was tolerated well for both routes of administration and underwent complete biotransformation to the active metabolite, penciclovir. Mean maximum plasma concentration of penciclovir was 1.3 μg/mL at 1.1 hours after oral administration of 5 mg/kg. Similar results were detected after rectal administration of 5 mg/kg. Mean maximum plasma concentration was 3.6 μg/mL at 0.66 hours after rectal administration of 15 mg/kg; this concentration was similar to results reported for humans receiving 7 mg/kg orally.

CONCLUSIONS AND CLINICAL RELEVANCE

Juvenile Asian elephants are susceptible to elephant endotheliotropic herpesvirus. Although most infections are fatal, case reports indicate administration of famciclovir has been associated with survival of 3 elephants. In Asian elephants, a dose of 8 to 15 mg of famciclovir/kg given orally or rectally at least every 8 hours may result in penciclovir concentrations that are considered therapeutic in humans.

摘要

目的

确定对亚洲象幼象(印度象)口服和直肠给予泛昔洛韦后喷昔洛韦的血浆药代动力学。

动物

6头健康亚洲象(5头雌性和1头雄性),年龄4.5至9岁,体重1646至2438千克。

方法

按照不完全交叉设计口服或直肠给予泛昔洛韦。三个治疗组,每组包括4头大象,分别接受单剂量泛昔洛韦(5毫克/千克,口服,或5或15毫克/千克,直肠给药);后续泛昔洛韦给药之间至少有12周的洗脱期。每次给药后采集系列血样。采用经过验证的液相色谱 - 质谱分析法分析样品中的泛昔洛韦和喷昔洛韦。

结果

两种给药途径对泛昔洛韦耐受性良好,且泛昔洛韦完全生物转化为活性代谢物喷昔洛韦。口服5毫克/千克后1.1小时,喷昔洛韦的平均最大血浆浓度为1.3微克/毫升。直肠给予5毫克/千克后检测到类似结果。直肠给予15毫克/千克后0.66小时,平均最大血浆浓度为3.6微克/毫升;该浓度与口服7毫克/千克的人类报告结果相似。

结论及临床意义

亚洲象幼象易感染象内皮嗜性疱疹病毒。虽然大多数感染是致命的,但病例报告表明给予泛昔洛韦与3头大象存活有关。在亚洲象中,至少每8小时口服或直肠给予8至15毫克/千克的泛昔洛韦可能会导致喷昔洛韦浓度达到人类治疗浓度。

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