Pharmacology of vanilloids at recombinant and endogenous rat vanilloid receptors

This study compared the actions of members of five different chemical classes of vanilloid agonists at the recombinant rat vanilloid VR1 receptor expressed in HEK293 cells, and at endogenous vanilloid receptors on dorsal root ganglion cells and sensory nerves in the rat isolated mesenteric arterial bed. In mesenteric beds, vanilloids elicited dose-dependent vasorelaxation with the rank order of potency: resiniferatoxin much greater than capsaicin = olvanil > phorbol 12-phenyl-acetate 13-acetate 20-homovanillate (PPAHV) > isovelleral. Scutigeral was inactive. Responses were abolished by capsaicin pretreatment and inhibited by ruthenium red. In VR1-HEK293 cells and dorsal root ganglion neurones, Ca2+ responses were induced by resiniferatoxin > capsaicin = olvanil > PPAHV; all four were full agonists. Isovelleral and scutigeral were inactive. The resiniferatoxin-induced Ca2+ response had a distinct kinetic profile. Olvanil had a Hill coefficient of similar to1 whilst capsaicin, resiniferatoxin and PPAHV had Hill coefficients of similar to2 in VR1-HEK293 cells. The capsaicin-induced Ca2+ response was inhibited in a concentration-dependent manner by ruthenium red > capsazepine > isovelleral. These data show that resiniferatoxin, capsaicin, olvanil and PPAHV, but not scutigeral and isovelleral, are agonists at recombinant rat VR1 receptors and endogenous vanilloid receptors on dorsal root ganglion neurones and in the rat mesenteric arterial bed. The vanilloids display the same relative potencies (resiniferatoxin > capsaicin = olvanil > PPAHV) in all of the bioassays. (C) 2002 Elsevier Science Inc. All rights reserved.