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阿法沙龙静脉注射和肌肉注射给猫后的药代动力学及效应

Pharmacokinetics and effects of alfaxalone after intravenous and intramuscular administration to cats.

作者信息

Rodrigo-Mocholí D, Escudero E, Belda E, Laredo F G, Hernandis V, Marín P

机构信息

a Faculty of Veterinary Medicine, Department of Veterinary Anaesthesia and Analgesia , University of Sydney , Camperdown , New South Wales , Australia.

b Faculty of Veterinary Medicine, Department of Pharmacology , University of Murcia , 30071 Espinardo, Murcia , Spain.

出版信息

N Z Vet J. 2018 Jul;66(4):172-177. doi: 10.1080/00480169.2018.1455541. Epub 2018 Apr 2.

Abstract

AIMS

To determine the pharmacokinetics, and anaesthetic and sedative effects of alfaxalone after I/V and I/M administration to cats.

METHODS

Six European shorthair cats, three males and three females, with a mean weight of 4.21 (SD 0.53) kg and aged 3.8 (SD 0.9) years were enrolled in this crossover, two-treatment, two-period study. Alfaxalone at a dose of 5 mg/kg was administered either I/V or I/M. Blood samples were collected between 2-480 minutes after drug administration and analysed for concentrations of alfaxalone by HPLC. The plasma concentration-time curves were analysed by non-compartmental analysis. Sedation scores were evaluated between 5-120 minutes after drug administration using a numerical rating scale (from 0-18). Intervals from drug administration to sit, sternal and lateral recumbency during the induction phase, and to head-lift, sternal recumbency and standing position during recovery were recorded.

RESULTS

The mean half-life and mean residence time of alfaxalone were longer after I/M (1.28 (SD 0.21) and 2.09 (SD 0.36) hours, respectively) than after I/V (0.49 (SD 0.07) and 0.66 (SD 0.16) hours, respectively) administration (p<0.05). Bioavailability after I/M injection of alfaxalone was 94.7 (SD 19.8)%. The mean intervals to sternal and lateral recumbency were longer in the I/M (3.73 (SD 1.99) and 6.12 (SD 0.90) minutes, respectively) compared to I/V (0 minutes for all animals) treated cats (p<0.01). Sedation scores indicative of general anaesthesia (scores >15) were recorded from 5-15 minutes after I/V administration and deep sedation (scores 11-15) at 20 and 30 minutes. Deep sedation was observed from 10-45 minutes after I/M administration. One cat from each group showed hyperkinesia during recovery, and the remainder had an uneventful recovery.

CONCLUSIONS AND CLINICAL RELEVANCE

Alfaxalone administered I/V in cats provides rapid and smooth induction of anaesthesia. After I/M administration, a longer exposure to the drug and an extended half life were obtained compared to I/V administration. Therefore I/M administration of alfaxalone could be a reliable, suitable and easy route in cats, taking into account that alfaxalone has a slower onset of sedation than when given I/V and achieves deep sedation rather than general anaesthesia.

摘要

目的

确定在猫静脉注射(I/V)和肌肉注射(I/M)阿法沙龙后的药代动力学以及麻醉和镇静效果。

方法

六只欧洲短毛猫,三只雄性和三只雌性,平均体重4.21(标准差0.53)千克,年龄3.8(标准差0.9)岁,被纳入这项交叉、双治疗、双周期研究。以5毫克/千克的剂量给猫静脉注射或肌肉注射阿法沙龙。在给药后2至480分钟采集血样,并用高效液相色谱法(HPLC)分析阿法沙龙的浓度。通过非房室分析对血浆浓度-时间曲线进行分析。在给药后5至120分钟使用数字评分量表(0至18分)评估镇静评分。记录诱导期从给药到侧卧、胸骨卧位和侧卧位的时间间隔,以及恢复期从给药到抬头、胸骨卧位和站立姿势的时间间隔。

结果

肌肉注射后阿法沙龙的平均半衰期和平均驻留时间(分别为1.28(标准差0.21)小时和2.09(标准差0.36)小时)比静脉注射后(分别为0.49(标准差0.07)小时和0.66(标准差0.16)小时)更长(p<0.05)。肌肉注射阿法沙龙后的生物利用度为94.7(标准差19.8)%。与静脉注射组(所有动物均为0分钟)相比,肌肉注射组猫达到胸骨卧位和侧卧位的平均时间间隔更长(分别为3.73(标准差1.99)分钟和6.12(标准差0.90)分钟)(p<0.01)。静脉注射后5至15分钟记录到表明全身麻醉的镇静评分(评分>15),20和30分钟时为深度镇静(评分11至15)。肌肉注射后10至45分钟观察到深度镇静。每组各有一只猫在恢复过程中出现运动亢进,其余猫恢复顺利。

结论及临床意义

在猫中静脉注射阿法沙龙可实现快速且平稳的麻醉诱导。与静脉注射相比,肌肉注射后药物暴露时间更长,半衰期延长。因此,考虑到阿法沙龙肌肉注射时镇静起效比静脉注射慢且达到的是深度镇静而非全身麻醉,肌肉注射阿法沙龙可能是猫一种可靠、合适且简便的给药途径。

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