首页> 外文期刊>Journal of medicinal food >Antiplatelet Effects of Rhus verniciflua Stokes Heartwood and Its Active Constituents-Fisetin, Butein, and Sulfuretin-in Rats
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Antiplatelet Effects of Rhus verniciflua Stokes Heartwood and Its Active Constituents-Fisetin, Butein, and Sulfuretin-in Rats

机译:鼠李木抚风心材及其活性成分-Fisetin,Butein和Sulfuretin-的抗血小板作用

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Rhus verniciflua stokes (RVS) is known to promote blood circulation by preventing blood stasis, although the active ingredients and the underlying mechanism are unclear. Platelets are the primary cells that regulate circulation and contribute to the development of diverse cardiovascular diseases by aggregation and thrombosis. The study assessed the antiplatelet activity of RVS and sought to identify the active constituents. Pretreatment of washed platelets with RVS heartwood extract blunted the aggregatory response of platelets to collagen. In the subfractions, fisetin, butein, and sulfuretin were identified as effective inhibitors of platelet aggregation by collagen, thrombin, and adenosine-5 '-diphosphate. Antiplatelet activities of all three compounds were concentration dependent, and fisetin had longer in vitro duration of action compared with butein or sulfuretin. Extracellular signal-regulated kinase (ERK) mitogen-activated protein kinase activation by collagen was prevented by fisetin, whereas butein and sulfuretin failed to inhibit ERK and p38 activation was not affected by any of the compounds. Rats orally administered 100 mg/(kg center dot day(-1)) fisetin for 7 days were resistant to arterial thrombosis, although total extract of RVS heartwood exhibited little effect at a dose of 1000 mg/(kg center dot day(-1)). RVS heartwood may have cardiovascular protective activity by inhibiting platelet aggregation. The active constituents are fisetin, butein, and sulfuretin, and fisetin is orally effective against thrombosis.
机译:尽管活性成分和潜在机制尚不清楚,但已知鼠李氏红景天(RVS)可通过阻止血瘀来促进血液循环。血小板是调节循环并通过聚集和血栓形成促进多种心血管疾病发展的主要细胞。该研究评估了RVS的抗血小板活性,并试图确定其活性成分。用RVS心材提取物预处理洗涤过的血小板会减弱血小板对胶原蛋白的聚集反应。在该部分中,通过胶原蛋白,凝血酶和5'-腺苷5'-二磷酸酯被鉴定为非瑟汀,丁酸和硫酸脂为血小板聚集的有效抑制剂。这三种化合物的抗血小板活性均与浓度有关,与非丁脂或硫酸脂相比,非瑟汀的体外作用时间更长。非瑟酮阻止了胶原蛋白对细胞外信号调节激酶(ERK)丝裂原活化的蛋白激酶的活化,而丁酮和硫酸盐则不能抑制ERK,p38活化不受任何化合物的影响。口服给予100 mg /(kg中心点日(-1))的非瑟定7天的大鼠对动脉血栓形成有抵抗力,尽管RVS心材的总提取物在1000 mg /(kg中心点日(-1)的剂量下几乎没有作用))。 RVS心材可能通过抑制血小板聚集而具有心血管保护作用。活性成分是非瑟汀,丁酮和硫汀,非瑟汀口服有效抗血栓形成。

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