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首页> 外文期刊>Phytomedicine : >Ginkgo biloba extract attenuates warfarin-mediated anticoagulation through induction of hepatic cytochrome P450 enzymes by bilobalide in mice
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Ginkgo biloba extract attenuates warfarin-mediated anticoagulation through induction of hepatic cytochrome P450 enzymes by bilobalide in mice

机译:银杏叶提取物通过银杏内酯诱导小鼠肝细胞色素P450酶减弱华法林介导的抗凝作用

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Ginkgo biloba extract (GBE) is a popular herbal ingredient used worldwide, but it is reported to induce bleeding as a serious adverse event. In this study we examined whether GBE induced spontaneous bleeding or accelerated warfarin anticoagulation via herb-drug interaction. Mice were given GBE or various active components of GBE orally for 5 days and blood coagulation parameters and hepatic cytochrome P450 enzymes (CYPs) were measured. Mice also received warfarin (racemate, (S)- or (R)-enantiomer) for the last 3 days of the 5-day regimen to examine GBE-warfarin interactions. Neither GBE (up to 1000 mg/kg) nor ginkgolide B (up to 140 mg/kg), a platelet-activating factor antagonist, influenced blood coagulation parameters. In contrast, GBE attenuated the anticoagulant action of warfarin. Bilobalide, a component of GBE that markedly induced hepatic CYPs including (S)-warfarin hydroxylase, showed similar effects. For (S)-warfarin, the anticoagulation action and the interaction with GBE was clear, while the influence on metabolism was greater for (R)-warfarin than for (S)-warfarin, which corresponded to the CYP types induced by GBE. These results suggest that GBE and ginkgolide B have no influence on blood coagulation in vivo, and that GBE attenuates the anticoagulation action of warfarin via induction of hepatic CYPs by bilobalide.
机译:银杏叶提取物(GBE)是一种在世界范围内广泛使用的草药成分,但据报道,它可引起出血,是一种严重的不良事件。在这项研究中,我们研究了GBE是否通过药草相互作用诱导自发性出血或加速华法林抗凝。给小鼠口服GBE或GBE的各种活性成分,持续5天,并测量凝血参数和肝细胞色素P450酶(CYP)。在为期5天的治疗方案的最后3天,小鼠还接受了华法林(外消旋物,(S)-或(R)-对映体)检查GBE-华法林的相互作用。血小板活化因子拮抗剂GBE(最高1000 mg / kg)和银杏内酯B(最高140 mg / kg)均不影响凝血参数。相反,GBE减弱了华法林的抗凝作用。 Bilobalide是GBE的一种成分,可明显诱导肝CYP,包括(S)-华法林羟化酶,其作用相似。对于(S)-华法林,抗凝作用和与GBE的相互作用是明确的,而(R)-华法林对代谢的影响大于(S)-华法林,这与GBE诱导的CYP类型相对应。这些结果表明GBE和银杏内酯B对体内的血液凝固没有影响,并且GBE通过银杏内酯诱导肝CYPs减弱了华法林的抗凝作用。

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