- 作者:Ester Carballo-Jane ; Lynn S. Gerckens ; Silvi Luell ; Allison S. Parlapiano ; Michael Wolff ; Steven L. Colletti ; James R. Tata ; Andrew K.P. Taggart ; M. Gerard Waters ; Jeremy G. Richman ; Margaret E. McCan
- 关键词:Acipimox ; Dog ; GPR109A ; Lipolysis ; Methods ; Nicotinic acid ; Rat ; Therapeutic index ; Vasodilatation
- 刊名:Journal of Pharmacological and Toxicological Methods
- 出版年:2007
- 出版时间:November-December 2007
- 年:2007
- 卷:56
- 期:3
- 页码:308-316
- 全文大小:1281 K
Methods
We have developed a vasodilatation model in the rat that measures changes in ear perfusion using laser Doppler flowmetry. In the dog, we have developed a model of vasodilatation measuring changes in red color values in the ear, using a spectrocolorimeter. Effects of GPR109A agonists on lipolysis were measured in both species after oral dosing of compounds, and measuring plasma levels of free fatty acids.
Results
In both rat and dog, GPR109A agonists induce dose- and time-dependent vasodilatation, similar to that observed in humans. Vasodilatation is inhibited in both species with cyclooxygenase inhibitors or a specific DP1 receptor antagonist, indicating that, as in man, nicotinic acid-induced vasodilatation in rats and dogs is mainly mediated by the release of PGD2.
Discussion
Our results show that both rat and dog are useful models for the characterization of GPR109A agonists. A therapeutic index for GPR109A agonists can be calculated in either species.