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Journal of the South African Veterinary Association

On-line version ISSN 2224-9435
Print version ISSN 1019-9128

J. S. Afr. Vet. Assoc. vol.79 n.3 Pretoria  2008

 

ARTICLE ARTIKEL

 

Thermal, cardiorespiratory and cortisol responses of impala (Aepyceros melampus) to chemical immobilisation with 4 different drug combinations

 

 

L C R MeyerI; R S HetemI; L G FickI; A MattheeII; D MitchellI; A FullerI

IBrain Function Research Group, School of Physiology, University of the Witwatersrand, 7 York Road, Parktown, 2193 South Africa
IINational Zoological Gardens Lichtenburg Game Breeding Centre, PO Box 716, Lichtenburg, 2740 South Africa

 

 


ABSTRACT

Thermometric data loggers were surgically implanted in 15 impala (Aepyceros melampus)to investigate the consequences of chemical capture. Impala were darted and chemically immobilised for 30 min with each of the following drug combinations: etorphine and azaperone; etorphine and medetomidine; thiafentanil and azaperone, and a thiafentanil medetomidine combination. During immobilisation, pulse oximeter readings, respiratory rhythm, the plane of immobilisation and plasma cortisol concentrations were measured and recorded. The impala developed an extremely high rise in body temperature, which peaked 20-30 min after reversal of the immobilisation. The magnitude of the rise in body temperature was similar for all the drug combinations (F = 0.8, P = 0.5), but the duration of the hyperthermia was shorter when the thiafentanil and azaperone combination was used (F = 3.35, P < 0.05). Changes in body temperature were related to the time that it tookfor an animal to become recumbent after darting (r2 = 0.45, P = 0.006) and not to the effect of the drug combination on time to recumbency (r2 = 0.29, P = 0.46). The relationship between time to recumbency and body temperature change, and also to plasma cortisol concentration (r2 = 0.67, P = 0.008), indicated that physiological consequences of capture were related to the duration of exposure to a stressor, and not to the pharmacology of the capture drugs. Although shorter time to recumbency in individuals resulted in the benefit of smaller stress responses and body temperature changes, those individuals were predisposed to developing hypoxia and possibly induction apnoea. When animals are chemically immobilised, reducing the thermal consequences of capture requires limiting the exposure of the animal to a psychological 'fright stress'.

Key words: body temperature, stress, etorphine, thiafentanil, medetomidine, azaperone, stress-induced hyperthermia, impala (Aepyceros melampus)


 

 

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Received: November 2007
Accepted: June 2008

 

 

* Author for correspondence. E-mail: leith.meyer@wits.ac.za

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