猫口服和肌肉注射美托咪定的比较

O.B. Ansah, M. Raekallio, O. Vainio
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引用次数: 20

摘要

美托咪定(200μg/kg)口服给药,并单独给7只猫服用。口服后(43.6±14.3分钟)达到血清药物峰值的速度比im给药后(21.6±10.0分钟)慢。口服给药后镇静和卧位的出现滞后。两种给药途径在血清峰值浓度、全身药物可用性或镇静程度方面没有统计学上的显著差异。然而,口服给药后,这些参数在个体之间存在相当大的差异。唾液分泌的程度与口服给药后的全身药物可用性呈负相关。在没有出现过度流涎的情况下,在相应的im给药后,获得的全身药物可用性和镇静深度与之相当,甚至更高。总之,口服美托咪定可诱导临床镇静,但当需要准确给药时,由于唾液分泌可能导致药物损失,口服途径可能不太可靠。
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Comparing oral and intramuscular administration of medetomidine in cats

Medetomidine (200 μg/kg) was administered orally and, on a seperate occasion, im to 7 cats. Peak serum drug concentrations were reached more slowly after oral (43.6 ± 14.3 min) than after im administration (21.6 ± 10.0 min). The onset of sedation and recumbency lagged after oral administration. There were no statistically significant differences between the 2 routes of administration in peak serum concentrations, systemic drug availability or extent of sedation. However, there was considerable variation in these parameters between individuals after oral administration. The extent of salivation correlated negatively with systemic drug availability after oral administration. Where excessive salivation did not occur, systemic drug availability and the depth of sedation were comparable to, or even higher than, were obtained after the corresponding im administrations. In conclusion, oral administration of medetomidine induced a clinical sedation but, when accurate dosing is a necessity, the oral route may not be very reliable due to possible drug losses through salivation.

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