Prolonged chemical restraint of walrus ( Odobenus rosmarus ) with etorphine supplemented with medetomidine

David Griffiths, E. Born, M. Acquarone
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引用次数: 0

Abstract

Physiological studies involving the use of isotopic water required chemical restraint of free-ranging walruses ( Odobenus rosmarus ) for several hours. In August 2000, six male walrus (total body mass: 1050–1550 kg) were immobilized in East Greenland by remote delivery of 8.0–9.8 mg of etorphine and subsequently restrained for up to 6.75 h by administration of medetomidine. The effects of etorphine were reversed with 10–24 mg diprenorphine. After termination of the etorphine-induced apnoea, lasting an average of 15.8 min (SD = 9.7, range = 9.5–35.2 min, n = 6), the animals were initially given 10–20 mg medetomidine intramuscularly. The initial dose was further augmented by 5 mg at intervals of 5 min. In two cases, when medetomidine was administered through a catheter inserted in the extradural vein, the animal became instantly apnoeic and regained respiratory function only after intravenous injection of the prescribed dose of the antagonist atipamezole and of the respiratory stimulant doxapram. After an average of 3.5 hours of immobilisation, rectal temperature began to increase and it is conceivable that this is the factor that will ultimately limit the duration of immobilisation. The animals became conscious and fully mobile shortly after an intravenous injection of a dose of atipamezole approximately twice the mass of the total dose of medetomidine given during the procedure followed by 400 mg of doxapram. It is concluded that medetomidine appears to be a suitable drug for chemical restraint of walruses for time-consuming procedures following initial immobilisation by etorphine. With animals of total body mass around 1,000–1,500 kg, the drug should be given intramuscularly in 10–20 mg increments (total mass 10–60 mg) until the breathing rate falls to approximately 1 min-1. At this level, breathing is maintained and animals do not respond to touch or injection.
乙托啡加美托咪定对海象的长效化学抑制作用
涉及使用同位素水的生理研究需要对自由放养的海象(Odobenus rosmarus)进行几个小时的化学约束。2000年8月,在东格陵兰岛,6只雄性海象(总体重:1050-1550公斤)通过远程给药8.0-9.8毫克埃托啡固定,随后通过给予美托咪定限制长达6.75小时。乙托啡的作用被10-24毫克的二丙诺啡逆转。乙托啡诱导的呼吸暂停结束后,平均持续15.8 min (SD = 9.7,范围= 9.5 ~ 35.2 min, n = 6),开始肌注美托咪定10 ~ 20 mg。初始剂量每隔5分钟增加5mg。在两个病例中,当通过硬膜外静脉插入导管给药时,动物在静脉注射处方剂量的拮抗剂阿替帕唑和呼吸兴奋剂多沙普兰后,立即出现呼吸暂停,并恢复呼吸功能。在平均3.5小时的固定后,直肠温度开始升高,可以想象这是最终限制固定时间的因素。在静脉注射一剂量的阿替帕唑(大约是美托咪定总剂量的两倍)和400毫克多沙普兰后,这些动物很快就变得有意识和完全活动。由此得出结论,美托咪定似乎是一种适合的药物,以化学约束海象的耗时程序后,最初由乙托啡固定。对于总体重在1,000-1,500 kg左右的动物,应以10-20 mg的增量(总质量10-60 mg)肌肉给药,直到呼吸速率降至约1分钟-1。在这个水平,动物保持呼吸,对触摸或注射没有反应。
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来源期刊
CiteScore
0.60
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0.00%
发文量
4
审稿时长
52 weeks
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