Effects of Ginkgo biloba extract (EGb 761) on arteriolar spasm in a rat cremaster muscle preparation.

O Stücker, C Pons, J P Duverger, K Drieu
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引用次数: 9

Abstract

The effects of an extract of Ginkgo biloba (EGb 761) on arteriolar spasm were confirmed using a preparation of rat cremaster muscle. When vasospasm was induced by rat serum, arteriolar constriction reached 25-30% of the initial diameter after 10 min. Intravenous injection of EGb 761 (30 mg/kg) 5 min after inducing spasm inhibited about 80% of this serum-induced vasoconstriction. As previous studies have shown that EGb 761 has an antiaggregatory effect on platelets, thrombin, serotonin (platelet-derived compounds that are present in the serum) and a thromboxane analogue (U46619) were also used to induce vasospasm. Administration of EGb 761 (30 mg/kg) 5 min after exposure of the preparation to serotonin (10(-3) M) or 10 min after exposure to thrombin (20 units) did not affect vasospasm induced by these agents. In contrast, treatment with this same dose of EGb 761 5 min after exposure of the preparation to U46619 (10(-4) M) abolished the arteriolar constriction induced by this agent in 15 min. The thromboxane/prostaglandin H2 receptor antagonist SQ29548 antagonized serum-induced vasospasm, indicating an involvement of thromboxane. Other experiments indicated that the effects of EGb 761 of counteracting vasospasm may be mediated in part by ginkgolide B, a triterpene constituent of the extract that is an antagonist of platelet-activating factor and in part by an 'NO-like' action of its proanthocyanidin constituents. Taken together, these results have revealed that EGb 761 treatment can antagonize the vasoconstrictor effect of thromboxane on arterioles. As thromboxane is implicated in many cardiovascular disorders, this property of EGb 761 may explain some of its beneficial clinical effects in such pathologies.

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银杏叶提取物(egb761)对大鼠肌制剂中小动脉痉挛的影响。
银杏叶提取物(egb761)对大鼠肌小动脉痉挛的影响得到了证实。当大鼠血清诱导血管痉挛时,10分钟后小动脉收缩达到初始直径的25-30%。在诱导痉挛后5分钟静脉注射EGb 761 (30 mg/kg)可抑制约80%的血清诱导血管收缩。先前的研究表明,EGb 761对血小板具有抗聚集作用,凝血酶、血清素(血清中存在的血小板衍生化合物)和血栓素类似物(U46619)也被用于诱导血管痉挛。在暴露于血清素(10(-3)M) 5分钟后或暴露于凝血酶(20单位)10分钟后给予EGb 761 (30 mg/kg),对这些药物引起的血管痉挛没有影响。相比之下,在U46619 (10(-4) M)暴露后5分钟,用相同剂量的EGb 761治疗15分钟后,该药物引起的小动脉收缩消失。血栓素/前列腺素H2受体拮抗剂SQ29548可拮抗血清诱导的血管痉挛,表明血栓素参与其中。其他实验表明,egb761对抗血管痉挛的作用可能部分是由银杏内酯B介导的,银杏内酯B是提取物的三萜成分,是血小板活化因子的拮抗剂,部分是由其原花青素成分的“no样”作用介导的。综上所述,这些结果表明,egb761治疗可以拮抗血栓素对小动脉的血管收缩作用。由于血栓素与许多心血管疾病有关,EGb 761的这一特性可能解释了它在这些疾病中的一些有益的临床作用。
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