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银杏叶提取物对血管平滑肌和心肌的电药理作用。

Electropharmacological actions of Ginkgo biloba extract on vascular smooth and heart muscles.

作者信息

Satoh Hiroyasu, Nishida Seiichiro

机构信息

Department of Pharmacology, Division of Crude and Herbal Medicine, Nara Medical University, Kashihara, Nara 634-8521, Japan.

出版信息

Clin Chim Acta. 2004 Apr;342(1-2):13-22. doi: 10.1016/j.cccn.2003.12.014.

DOI:10.1016/j.cccn.2003.12.014
PMID:15026263
Abstract

Ginkgo biloba extract (GBE) is composed mostly of two constituents: One is terpenoids (such as bilobalide, ginkgolides A, B and C), and the other is flavonoids (such as quercetin and rutin). After oral administration of GBE (160 mg) to healthy volunteers, the plasma concentrations of ginkgolides A and B and bilobalide are 41.8, 5.6 and 37.6 ng/ml, respectively. GBE and bilobalide cause a potent concentration-dependent relaxation. NG-Monomethyl-l-arginine acetate (l-NMMA), an NO synthesis inhibitor, reduces the vasodilation induced by GBE. Furthermore, the vasorelaxation of GBE is attenuated in Ca2+-free medium. Bilobalide possesses similar mechanisms. The other constituents also produce vasorelaxation. On the other hand, all the compounds markedly modify the action potential configuration in guinea pig ventricular cardiomyocytes. GBE prolongs the action potential duration (APD), whereas bilobalide shortens the APD. In patch-clamp experiments, GBE markedly inhibits the Ca2+ current (ICa), the delayed rectifier K+ current (IK) and the inwardly rectifying K+ current (IK1). On the contrary bilobalide enhances the ICa and IK currents concentration-dependently. The other constituents do not cause their actions in a uniform direction. In the rat sino-atrial (SA) node, GBE causes a negative chronotropic effect. These results indicate that GBE and the constituents produce effective electropharmacological actions in the cardiomyocytes and cause vasodilation, mainly due to the inhibitions of Ca2+ influx through the Ca2+ channel and the activation of NO release in the endothelium and aortic vascular muscles.

摘要

银杏叶提取物(GBE)主要由两种成分组成:一种是萜类化合物(如白果内酯、银杏内酯A、B和C),另一种是黄酮类化合物(如槲皮素和芦丁)。给健康志愿者口服GBE(160毫克)后,银杏内酯A、B和白果内酯的血浆浓度分别为41.8、5.6和37.6纳克/毫升。GBE和白果内酯可引起有效的浓度依赖性舒张。NO合成抑制剂N-单甲基-L-精氨酸醋酸盐(L-NMMA)可降低GBE诱导的血管舒张。此外,在无钙培养基中,GBE的血管舒张作用减弱。白果内酯具有类似的机制。其他成分也能产生血管舒张作用。另一方面,所有这些化合物都能显著改变豚鼠心室心肌细胞的动作电位形态。GBE可延长动作电位时程(APD),而白果内酯则缩短APD。在膜片钳实验中,GBE可显著抑制钙电流(ICa)、延迟整流钾电流(IK)和内向整流钾电流(IK1)。相反,白果内酯可浓度依赖性地增强ICa和IK电流。其他成分的作用方向并不一致。在大鼠窦房结中,GBE可产生负性变时作用。这些结果表明,GBE及其成分在心肌细胞中产生有效的电药理作用并引起血管舒张,主要是由于抑制了通过钙通道的钙内流以及激活了内皮和主动脉血管平滑肌中的NO释放。

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