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萘醌类化合物白花丹素通过P2Y1-磷脂酶C信号通路抑制二磷酸腺苷诱导的大鼠血小板聚集。

The naphthoquinone plumbagin suppresses ADP-induced rat platelet aggregation through P2Y1-PLC signaling pathway.

作者信息

Zhang Qianrui, Liao Xiaoyan, Wu Fangjian

机构信息

Department of Pharmacy, General Hospital of the Yangtze River Shipping, Wuhan, China.

School of Pharmaceutical Science, Wuhan University, Wuhan, China.

出版信息

Pak J Pharm Sci. 2017 Mar;30(2(Suppl.)):573-578.

Abstract

Plumbagin (PLB) isolated from Plumbago zeylanica L (Plumbaginaceae) was evaluated for the suppressive effect and mechanism on ADP induced rat platelet aggregation. Adult male SD rats were randomly divided into control group, clopidogrel group, PLB 25mg/kg group and PLB 50mg/kg group. Clopidogrel (13.5mg/kg per day) and PLB (25 and 50mg/kg per day) were orally given to experimental rats by gavage for seven consecutive days. The antiplatelet properties were assessed by measuring the ADP-induced platelet aggregation rate (Agg). The level of cAMP in platelets before aggregation was determined by ELISA. The protein expression of pAkt, Akt, pPLC β3 and PLC β3 in platelets was measured by western blot. Our data indicated that PLB (25 and 50mg/kg) significantly inhibited ADP-induced rat platelet aggregation as well as clopidogrel (13.5mg/kg) in a dose dependent manner compared with the control group. PLB (25 and 50mg/kg) remarkably reduced the ADP-induced PLC β3 phosphorylation but not Akt in platelets as compared with the control group. The present study suggests that PLB exerts a suppressive effect on ADP-induced rat platelet aggregation, at least in part, through P2Y-PLC signaling pathway.

摘要

从白花丹(白花丹科)中分离得到的白花丹素(PLB),针对其对二磷酸腺苷(ADP)诱导的大鼠血小板聚集的抑制作用及机制进行了评估。成年雄性SD大鼠被随机分为对照组、氯吡格雷组、PLB 25mg/kg组和PLB 50mg/kg组。连续7天通过灌胃法给实验大鼠口服氯吡格雷(每天13.5mg/kg)和PLB(每天25和50mg/kg)。通过测量ADP诱导的血小板聚集率(Agg)来评估抗血小板特性。采用酶联免疫吸附测定法(ELISA)测定聚集前血小板中cAMP的水平。通过蛋白质免疫印迹法检测血小板中pAkt、Akt、pPLC β3和PLC β3的蛋白表达。我们的数据表明,与对照组相比,PLB(25和50mg/kg)以剂量依赖性方式显著抑制ADP诱导的大鼠血小板聚集,效果与氯吡格雷(13.5mg/kg)相当。与对照组相比,PLB(25和50mg/kg)显著降低了ADP诱导的血小板中PLC β3磷酸化,但对Akt无影响。本研究表明,PLB至少部分通过P2Y-PLC信号通路对ADP诱导的大鼠血小板聚集发挥抑制作用。

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