Evaluation of etorphine reversed by diprenorphine for the immobilisation of free-ranging Atlantic walrus ( Odobenus rosmarus rosmarus L.)

M. Acquarone, E. Born, David Griffiths, L. O. Knutsen, Ø. Wiig, I. Gjertz
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引用次数: 5

Abstract

To date no problem-free method exists for the immobilisation of free‑ranging walruses ( Odobenus rosmarus ). In the period 1989-2001, 69 immobilisations with etorphine HCl were performed by remote darting of 41 individual free-ranging adult Atlantic walruses ( O. r. rosmarus ), with body masses 633 ‑ 1883 kg, as a rerequisite for the attachment of radio tracking and dive recording instruments, and for studies of metabolism. Ten individuals were immobilised several times. We present data on these 69 immobilisations and evaluate the method. Full immobilisation was achieved in 58 cases (84 %). The animals were insufficiently restrained in 6 cases (9 %) and 5 animals died (7 %) following the immobilisation. The animals were fully immobilised and approachable after 5 min (n = 38, range = 1.9 ‑ 12.4 min, SD = 2.2) with a dose of etorphine of 6.1 μg/kg (range 2.4 ‑ 12.6 μg /kg, SD = 2.4). Induction time was negatively correlated with the dosage of etorphine. Etorphine-induced apnoea lasted 13.7 min (n = 36, range 17.0 ‑ 26.7 min, SD = 5.1) and was reversed by multiple doses of the antagonist diprenorphine HCl. The first dose of antagonist of 12.2 mg (n = 39, range 6.0 ‑ 21.0 mg, SD = 3.5) was administered 8.4 min (n = 38, range 4.7 ‑ 18.0 min, SD = 2.8) after injection of the agonist. The total dose of diprenorphine per animal ranged between 7.7 and 41.7 μg/kg (n = 31, mean  = 17.2 μg/kg, SD = 7.5). For some animals blood pH values were measured following the apnoea and reached low levels (min pH 6.8). For animals that were immobilised several times there were no indications of changed sensitivity to etorphine as reflected in unchanged induction times. Mortalities could neither be related to the doses of agonist and antagonist, nor to the times of administration of the drugs. From this (n = 69) and other (n = 103) studies involving etorphine immobilisation of walruses (both Atlantic and Pacific) the overall success rate is 83 % (8 % casualty rate). We conclude that the combination etorphine‑ diprenorphine is suitable for both single and multiple immobilisations of walruses provided that (a) a casualty rate of 7-8% is acceptable (b) the antagonist diprenorphine is administered fast and well into a tissue with good blood irrigation, and (c) the animal is promptly intubated endotracheally to facilitate the restoration of breathing after drug-induced apnoea.
二丙诺啡逆转乙托啡对自由放养大西洋海象固定作用的评价
迄今为止,对于自由放养的海象(Odobenus rosmarus)的固定,还没有没有问题的方法。1989-2001年期间,对41只体重633 - 1883千克的自由放养的成年大西洋海象(O. r. rosmarus)进行了69次盐酸艾托啡固定,这是安装无线电跟踪和潜水记录仪器以及研究新陈代谢的必要条件。10个人被多次固定。我们提出了这69个固定和评估方法的数据。完全固定58例(84%)。6例(9%)动物未被充分约束,5例(7%)动物在固定后死亡。在给药剂量为6.1 μg/kg(范围为2.4 - 12.6 μg/kg, SD = 2.4)的情况下,5 min (n = 38,范围为1.9 - 12.4 min, SD = 2.2)使动物完全固定并可接近。诱导时间与乙托啡用量呈负相关。乙托啡诱导的呼吸暂停持续13.7 min (n = 36,范围17.0 ~ 26.7 min, SD = 5.1),可通过多剂量拮抗剂盐酸二丙诺啡逆转。第一剂拮抗剂为12.2 mg (n = 39,范围6.0 ~ 21.0 mg, SD = 3.5),注射后8.4 min (n = 38,范围4.7 ~ 18.0 min, SD = 2.8)给药。每只动物双丙诺啡总剂量范围为7.7 ~ 41.7 μg/kg (n = 31, mean = 17.2 μg/kg, SD = 7.5)。一些动物的血液pH值在呼吸暂停后测量,达到低水平(最小pH值6.8)。对于固定多次的动物,没有迹象表明对乙托啡的敏感性发生了变化,这反映在不变的诱导时间上。死亡率既与激动剂和拮抗剂的剂量无关,也与给药时间无关。从这个(n = 69)和其他(n = 103)涉及吗啡固定海象(大西洋和太平洋)的研究来看,总体成功率为83%(伤故率为8%)。我们的结论是,联合使用乙托啡-二丙诺啡适用于海象的单次和多次固定,前提是:(a)伤伤率为7-8%是可接受的;(b)拮抗剂二丙诺啡快速且良好地进入组织,并有良好的血液冲洗;(c)动物及时气管内插管,以促进药物引起的呼吸暂停后呼吸的恢复。
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来源期刊
CiteScore
0.60
自引率
0.00%
发文量
4
审稿时长
52 weeks
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