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Plant extracts inhibit ADP-induced platelet activation in humans: their potential therapeutic role as ADP antagonists

机译:植物提取物抑制人体内ADP诱导的血小板活化:其作为ADP拮抗剂的潜在治疗作用

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摘要

Adenosine diphosphate (ADP) plays a pivotal role in platelet activation. Platelet hyperactivity is associated with vascular disease and also has a key role in haemostasis and thrombosis. ADP activates platelets through three purinoceptor subtypes, the Gq-coupled P2Y1 receptor, Gi-coupled P2Y12 receptor and P2X1 ligand-gated cation channel. Platelet ADP purinergic receptors are therefore suitable targets for antiplatelet drugs. Thienopyridines such as clopidogrel and ticlopidine, as well as other ADP receptor antagonists like prasugrel, ticagrelor, cangrelor and elinogrel have demonstrated clinical benefits via the inhibition of the selective purinergic ADP receptor, P2Y12. However, they still have limitations in their mode of action and efficacy, like increased risk of bleeding. Thus, the ongoing pursuit to develop newer and more effective antiplatelet agents continues. There is a growing interest in the purinergic antiplatelet properties exhibited by plant extracts. This article considers the following: pomolic acid isolated from Licania pittieri, brazilin isolated from the heartwood of Caesalpinia sappan L, phylligenin isolated from the twigs of Muraltia vulpina, bark oil of Gonystylus velutinus, seed and bark extracts from Aesculus hippocastanum L. and red wine phenolics and catechins isolated from green tea. Moreover, the method used to investigate platelet purinergic receptors should be considered, since using a more sensitive, high-resolution platelet sizer can sometimes detect platelet variations when the light transmission method was not able to do so. The exact mechanisms by which these plant extracts work need further investigation. They all however inhibit ADP-induced activation in human platelets. This could explain, at least in part, the protective effect of plant extracts as antiplatelet agents.
机译:二磷酸腺苷(ADP)在血小板活化中起关键作用。血小板多动症与血管疾病有关,并且在止血和血栓形成中也起关键作用。 ADP通过三种嘌呤受体亚型(Gq偶联的P2Y1受体,Gi偶联的P2Y12受体和P2X1配体门控的阳离子通道)激活血小板。因此,血小板ADP嘌呤能受体是抗血小板药物的合适靶标。噻吩并吡啶类(如氯吡格雷和噻氯匹定)以及其他ADP受体拮抗剂(如普拉格雷,替卡格雷,坎格雷洛和依诺格雷)已通过抑制选择性嘌呤能ADP受体P2Y12证明了其临床益处。但是,它们的作用方式和功效仍然存在局限性,例如出血风险增加。因此,开发新的和更有效的抗血小板药的持续追求。人们对植物提取物的嘌呤能抗血小板特性越来越感兴趣。本文考虑以下内容:从Licania pittieri分离得到的波莫酸,从Caesalpinia sappan L的心材分离出的巴西棕榈酸,从Muraltia vulpina的嫩枝中分离出的phylligenin,Gonystylus velutinus的树皮油,Aesculus Hippocastanum L.的种子和树皮提取物以及红酒。从绿茶中分离出的酚类和儿茶素。此外,应考虑用于研究血小板嘌呤能受体的方法,因为使用更灵敏,更高分辨率的血小板分选仪有时可以在光透射法无法检测血小板变化的情况下进行检测。这些植物提取物工作的确切机制需要进一步研究。但是它们都抑制人血小板中ADP诱导的活化。这至少可以部分解释植物提取物作为抗血小板药的保护作用。

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