Anesthesia of Grizzly Bears Using Xylazine-zolazepam-tiletamine or Zolazepam-tiletamine

Article published in Ursus. Citation only.

Abstract

The immobilization features and physiological effects of combinations of xylazine-zolazepam-tiletamine (XZT) and zolazepam-tiletamine (ZT) were compared in 46 wild grizzly bears (Ursus arctos) handled during 90 captures. Although induction time was similar between drugs, induction dosage and volume were less with XZT than with ZT. Induction of immobilization with XZT was predictable and smooth, and muscle relaxation was good during the period of immobilization. XZT was tolerated safely at 2-3 times the recommended dosage of 6-7 mg/kg (xylazine at 2.4-2.8 mg/kg + ZT at 3.6-4.2 mg/kg with X and ZT mixed in a 2:3 ratio). Bears anesthetized with XZT had slower pulse rates and higher rectal temperatures than bears anesthetized with ZT. The risk of hyperthermia at higher ambient temperatures (≥25°C) was of potential concern with XZT. Although transient hypoxemia (hemoglobin oxygen saturation [SpO2] ≤ 85%) developed immediately following induction in some bears, it was not severe enough to pose significant health risk. The provision of supplementary oxygen during hypoxemia resulted in increased SpO2 and decreased pulse rate. Bears anesthetized with XZT had higher serum glucose concentrations than bears anesthetized with ZT, a finding likely explained by the α2- adrenergic effects of xylazine to increase hepatic glucose production and decrease pancreatic release of insulin. Although the time to complete reversal of effects was highly variable, the effects of XZT anesthesia could be reversed with the α2-antagonist drug yohimbine.

Citation

Cattet, M. R. L., Caulkett, N. A., & Stenhouse, G. B. (2003). Anesthesia of grizzly bears using xylazine-zolazepam-tiletamine or zolazepam-tiletamine. Ursus, 14(1), 88–93. doi:10.2307/3872961