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Horm Metab Res 1988; 20(1): 32-36
DOI: 10.1055/s-2007-1010742
ORIGINALS
Basic
© Georg Thieme Verlag, Stuttgart · New York

Enhanced Apomophine-Induced Hypothermia in Alloxan-Treated Rats

J. E. Bjorenson1 , R. M. Quock2
  • 1Department of Comparative Biosciences, University of Wisconsin-Madison, School of Veterinary Medicine, Madison, Wisconsin, U.S.A.
  • 2Department of Basic Sciences, Marquette University School of Dentistry, Milwaukee, Wisconsin, U.S.A.
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Publication History

1986

1987

Publication Date:
14 March 2008 (online)

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Summary

Previous studies have indicated that drug-induced experimental diabetes is associated with increased receptor binding in the rat brain. The purpose of this study was to determine whether the dopamine receptor agonist apomorphine (APO) might produce an accentuated hypothermic response in rats rendered diabetic by alloxan (ALX) treatment. In a previous study, however, the only controls used were ALX-treated rats that failed to develop glycosuria. Therefore, in this study, APO (0.5 mg/kg IP) was administered to ALX-diabetic and non-diabetic as well as saline-treated control rats to ascertain whether the APO responsiveness of ALX-non-diabetic rats was comparable to that of saline control animals. ALX-diabetic rats experienced significantly greater hypothermic response to APO than did the saline control animals. Although ALX-non-diabetic rats were similar to the saline control animals in body weight and blood glucose levels, they too were hyperresponsive to APO. These findings indicate that pancreatic injury from ALX, while not always sufficiently severe to produce overt diabetes, does appear to induce an hyperresponsiveness to APO-induced hypothermia in a manner similar to that observed in severely diabetic animals.

Key-Words

Apomorphine - Dopamine Receptors - Alloxan - Experimental Diabetes - Hypothermia