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首页> 外文期刊>Journal of Ethnopharmacology: An Interdisciplinary Journal Devoted to Bioscientific Research on Indigenous Drugs >Tanshinone IIA, a major component of Salvia milthorriza Bunge, inhibits platelet activation via Erk-2 signaling pathway
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Tanshinone IIA, a major component of Salvia milthorriza Bunge, inhibits platelet activation via Erk-2 signaling pathway

机译:丹参IIA是丹参中的主要成分,可通过Erk-2信号通路抑制血小板活化

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Ethnopharmacological relevance The roots of Salvia milthorriza Bunge (Lamiaceae) known as "Danshen", are used in Traditional Chinese Medicine as a remedy for activating blood and eliminating stasis. TIIA, a diterpenoid of Salvia milthorriza, is one of active components in Danshen that exhibits a significant improvement of the blood flow in the coronary circulatory system and a reduction of myocardial infarction. However, its effect on platelet and underlying mechanism remains largely unknown. On this basis, this compound could be a promising agent to improve blood viscosity and microcirculation and to prevent CVD. Materials and methods In order to investigate the effects of TIIA on platelet functionality and its interaction with various platelet activation pathways, rat PRP were incubated with TIIA for 1 min at 37 °C prior the addition of the stimuli (ADP or collagen). Aggregation was monitored in a light transmission aggregometer measuring changes in turbidity with continuous observation up to 10 min after the addition of the stimuli. MAPK signaling pathway and tubulin acetylation were analyzed by a Western blot technique. The effect of the TIIA was also studied in vivo on bleeding time in mice. Results TIIA selectively inhibited rat platelet aggregation induced by reversible ADP stimuli (3 μM) in a concentration-dependent manner (0.5-50 μM). Nevertheless, TIIA was less active against the irreversible stimuli induced by ADP (10 μM) and collagen (10 μg/mL). Moreover, experiments performed on platelet lysates collected at different time-point after the addition of the stimuli shown that TIIA modulated tubulin acetylation and inhibited Erk-2 phosphorylation. Concomitantly, TIIA administrated i.p. At 10 mg/kg significantly amplified the mice bleeding time with an increase of 58% compared to its control (2.06±0.29 min vs 1.30±0.07). ASA was used as reference drug for in vitro and in vivo experiments. Conclusions This study clarifies the intracellular signaling pathway involved in antiplatelet action of TIIA and also gives preliminary evidences for its anticoagulant activity. On this basis, this compound could be a promising agent to improve blood viscosity and microcirculation and to prevent CVD.
机译:民族药理学相关性丹参(丹参)的根在传统中药中被用作活血化瘀的药物。 TIIA是丹参中的二萜类化合物,是丹参中的活性成分之一,在冠状动脉循环系统中表现出明显的血流改善和心肌梗塞的减少。然而,其对血小板及其潜在机制的影响仍是未知之数。在此基础上,该化合物可能是改善血液粘度和微循环并预防CVD的有前途的药物。材料和方法为了研究TIIA对血小板功能的影响及其与各种血小板激活途径的相互作用,在添加刺激物(ADP或胶原蛋白)之前,将大鼠PRP与TIIA在37°C孵育1分钟。加入光刺激后,在长达10分钟的连续观察过程中,通过光透射聚集仪监测聚集,以测量浊度变化。通过蛋白质印迹技术分析了MAPK信号通路和微管蛋白乙酰化。还在体内研究了TIIA对小鼠出血时间的影响。结果TIIA以浓度依赖性(0.5-50μM)选择性抑制可逆ADP刺激(3μM)诱导的大鼠血小板聚集。尽管如此,TIIA对ADP(10μM)和胶原蛋白(10μg/ mL)诱导的不可逆刺激的活性较低。此外,在添加刺激后在不同时间点收集的血小板裂解物上进行的实验表明,TIIA调节微管蛋白的乙酰化并抑制Erk-2磷酸化。同时,TIIA管理了i.p.与对照相比,以10 mg / kg的剂量可明显增加小鼠的出血时间,增加58%(2.06±0.29分钟vs.1.30±0.07)。 ASA用作体外和体内实验的参考药物。结论本研究阐明了TIIA的抗血小板作用涉及的细胞内信号传导途径,并为其抗凝活性提供了初步的证据。在此基础上,该化合物可能是改善血液粘度和微循环并预防CVD的有前途的药物。

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