THE VASORELAXANT EFFECT OF EVODIAMINE IN RAT ISOLATED MESENTERIC-ARTERIES - MODE OF ACTION

被引:105
作者
CHIOU, WF
CHOU, CJ
SHUM, AYC
CHEN, CF
机构
[1] NATL YANG MING MED COLL,DEPT PHARMACOL,SHIH PAI,TAIWAN
[2] NATL RES INST CHINESE MED,TAIPEIHSIEN,TAIWAN
关键词
EVODIAMINE; ENDOTHELIUM; CA2+ CHANNELS; K+ CHANNELS; MESENTERIC ARTERY;
D O I
10.1016/0014-2999(92)90039-7
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
The roles of the endothelium, Ca2+ and K+ fluxes in the evodiamine-induced attenuation of vascular contractile responses to vasoactive agents were examined. The results showed that: (1) in rat mesenteric artery rings, evodiamine elicited a concentration-dependent attenuation in the contractile response generated by phenylephrine. The inhibitory potency was greater for intact than for endothelium-denuded preparations. Thus, the vasodilator action of evodiamine appeared to be partially endothelium-interactive (dependent). (2) Evodiamine pretreatment had a greater inhibitory effect on the phenylephrine-induced tonic contraction (via Ca2+ influx) than on the phasic contraction (via Ca2+ release). In addition, evodiamine was more potent to inhibit the restoration by CaCl2 of contractile responses to phenylephrine than a potassium depolarizing solution in media that had been kept calcium-free. These results suggest that block of the Ca2+ influx through receptor-mediated Ca2+ channels may be the major mechanism underlying the vasodilator effect of evodiamine. (3) A K+ channel blocker, tetraethylammonium, almost completely abolished the vasodilatation induced by minoxidil (a known K+ channel opener) but not evodiamine. The possible involvement of K+ channel activation of the vasodilator effect produced by evodiamine was therefore excluded.
引用
收藏
页码:277 / 283
页数:7
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