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Hydroxyl Group and Vasorelaxant Effects of Perillyl Alcohol Carveol Limonene on Aorta Smooth Muscle of Rats

机译:紫苏醇香芹醇柠檬烯对大鼠主动脉平滑肌的羟基和血管舒张作用

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摘要

The present study used isometric tension recording to investigate the vasorelaxant effect of limonene (LM), carveol (CV), and perillyl alcohol (POH) on contractility parameters of the rat aorta, focusing in particular on the structure-activity relationship. LM, CV, and POH showed a reversible inhibitory effect on the contraction induced by electromechanical and pharmacomechanical coupling. In the case of LM, but not CV and POH, this effect was influenced by preservation of the endothelium. POH and CV but not LM exhibited greater pharmacological potency on BayK-8644-induced contraction and on electromechanical coupling than on pharmacomechanical coupling. In endothelium-denuded preparations, the order of pharmacological potency on electrochemical coupling was LM < CV < POH. These compounds inhibited also, with grossly similar pharmacological potency, the contraction induced by phorbol ester dibutyrate. The present results suggest that LM, CV and POH induced relaxant effect on vascular smooth muscle by means of different mechanisms likely to include inhibition of PKC and IP3 pathway. For CV and POH, hydroxylated compounds, it was in electromechanical coupling that the greater pharmacological potency was observed, thus suggesting a relative specificity for a mechanism likely to be important in electromechanical coupling, for example, blockade of voltage-dependent calcium channel.
机译:本研究使用等距张力记录来研究柠檬烯(LM),香芹酚(CV)和紫苏醇(POH)对大鼠主动脉收缩性参数的血管舒张作用,特别是在结构-活性关系上。 LM,CV和POH对机电和药效耦合引起的收缩表现出可逆的抑制作用。对于LM而言,但对CV和POH则不然,这种作用受内皮保存的影响。 POH和CV而不是LM对BayK-8644诱导的收缩和机电耦合表现出比药效耦合更高的药理作用。在内皮剥蚀的制剂中,药理作用对电化学偶联的顺序为LM

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