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槲皮素和 3',4'-二羟基黄酮醇的治疗抑制血小板功能并减少体内血栓形成。

Treatment with quercetin and 3',4'-dihydroxyflavonol inhibits platelet function and reduces thrombus formation in vivo.

机构信息

School of Medical Sciences, RMIT University, Melbourne, VIC, Australia.

出版信息

J Thromb Thrombolysis. 2013 Jul;36(1):50-7. doi: 10.1007/s11239-012-0827-2.

DOI:10.1007/s11239-012-0827-2
PMID:23070586
Abstract

Flavonols are polyphenolic compounds with reported cardiovascular benefits and have been shown to exhibit antiplatelet properties in vitro. While some studies have shown inhibition of platelet aggregation following dietary supplementation with flavonol rich foods, few studies have assessed the ability of flavonols to inhibit platelet mediated thrombus generation in vivo. Furthermore, the duration of benefit and the influence of different dosing regimens remain unclear. In this study we investigate the ability of two structurally related flavonols; quercetin (Que) and 3',4'-dihydroxyflavonol (DiOHF) to inhibit platelet aggregation, platelet granule exocytosis and vessel occlusion in a well characterized mouse model of platelet mediated arterial thrombosis. We investigated the effect of a single 6 mg/kg intravenous bolus and daily 6 mg/kg intraperitoneal doses over seven consecutive days. Carotid artery blood flow after injury was better maintained in mice treated with both Que and DiOHF when compared to the vehicle for both dosage regimens. This improved blood flow corresponded to inhibition of platelet aggregation and platelet dense granule exocytosis following chemical stimulation of PAR4. We therefore provide evidence of inhibition of platelet-mediated arterial thrombosis by flavonols in vivo, and demonstrate that this effect persists for at least 24 h after the last intraperitoneal dose. These data suggest a potential clinical role for flavonols as anti-platelet therapy.

摘要

类黄酮是具有报道的心血管益处的多酚化合物,已被证明具有体外抗血小板特性。虽然一些研究表明,富含类黄酮的食物的饮食补充后会抑制血小板聚集,但很少有研究评估类黄酮抑制体内血小板介导的血栓生成的能力。此外,获益的持续时间和不同剂量方案的影响仍不清楚。在这项研究中,我们研究了两种结构相关的类黄酮;槲皮素(Que)和 3',4'-二羟基黄酮(DiOHF)抑制血小板聚集、血小板颗粒胞吐作用和血管闭塞的能力,在一种特征明确的血小板介导的动脉血栓形成的小鼠模型中。我们研究了单次 6mg/kg 静脉推注和连续 7 天每天 6mg/kg 腹腔内剂量的影响。与两种剂量方案的载体相比,Que 和 DiOHF 治疗的小鼠在损伤后的颈动脉血流得到更好的维持。这种改善的血流与 PAR4 化学刺激后血小板聚集和血小板致密颗粒胞吐的抑制相对应。因此,我们提供了体内类黄酮抑制血小板介导的动脉血栓形成的证据,并证明这种作用在最后一次腹腔内剂量后至少持续 24 小时。这些数据表明类黄酮作为抗血小板治疗具有潜在的临床作用。

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