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三七皂甙单体2A-1-1对人血小板聚集和钙内流的作用
引用本文:曾福仁,尹松梅,谢双峰,聂大年,马丽萍,冯坚红,徐立卓,关永源. 三七皂甙单体2A-1-1对人血小板聚集和钙内流的作用[J]. 中华血液学杂志, 2004, 25(9): 544-547
作者姓名:曾福仁  尹松梅  谢双峰  聂大年  马丽萍  冯坚红  徐立卓  关永源
作者单位:1. 510120,广州,中山大学第二附属医院血液内科
2. 中山大学中山医学院药理学教研室
基金项目:广东省自然科学基金团队研究项目 (2 0 0 0 ),广东省科技计划资助项目 (2 0 0 3C3 2 70 9),广东省重点科技攻关项目(99M0 4810G)
摘    要:目的观察三七皂甙单体2A-1-1对人血小板聚集和钙内流的影响,并探讨其对受体操纵性钙通道的作用.方法比浊法测定血小板聚集;Fura-2/Am荧光探针双波长测定细胞胞浆游离钙浓度,观察2A-1-1、硝苯地平、SK&F96365对二磷酸腺苷(ADP)、环匹阿尼酸(CPA)介导的人血小板钙内流的变化.结果硝苯地平(20μmol/L)不能抑制ADP诱导的血小板聚集,不能抑制ADP或CPA介导的血小板钙内流;SK&F96365(20μmol/L)可以抑制ADP诱导的血小板聚集,抑制率为59.83%;SK&F96365(15μmol/L)可以抑制CPA和ADP介导的钙内流;2A-1-1(5,10,20,μmol/L)可抑制ADP诱导的血小板聚集,抑制率分别为47.06%,53.47%,71.52%;2A-1-1(10,20 μmol/L)可抑制CPA和ADP介导的钙内流.结论三七皂甙单体2A-1-1能抑制人血小板聚集,抑制血小板受体操纵性钙通道,从而抑制钙内流,有抗血小板作用.

关 键 词:钙通道阻滞药  血小板  聚集  
修稿时间:2003-12-08

Effects of 2A-1-1 on the aggregation and Ca2+ influx of platelets
Fu-ren Zeng,Song-mei Yin,Shuang-feng Xie,Da-nian Nie,Li-ping Ma,Jian-hong Feng,Li-zhuo Xu,Yong-yuan Guan. Effects of 2A-1-1 on the aggregation and Ca2+ influx of platelets[J]. Chinese Journal of Hematology, 2004, 25(9): 544-547
Authors:Fu-ren Zeng  Song-mei Yin  Shuang-feng Xie  Da-nian Nie  Li-ping Ma  Jian-hong Feng  Li-zhuo Xu  Yong-yuan Guan
Affiliation:Department of Hematology, 2nd affiliated hospital of Sun yat-sen University, Guangzhou 510120, China.
Abstract:OBJECTIVE: To explore the effects of 2A-1-1 (purified component from Panax notoginsengs saponins) on the aggregation of and Ca2+ influx into human platelets. METHODS: The aggregation of platelets was tested by nephelometry, Fura-2 fluorescent technique was used for detecting cell [Ca2+]i. The effects of 2A-1-1, nifedipine and SK&F96365 on Ca(2+) influx into human platelets induced by ADP or CPA were observed separately. RESULTS: Nifedipine (< 20 micromol/L) could not inhibit platelet aggregation induced by ADP or the Ca(2+) influx induced by ADP or CPA. SK&F96365 at 20 micromol/L could inhibit the maximal aggregation of platelets induced by ADP with a inhibitory rate of 59.83%, at 15 micromol/L could inhibit the Ca2+ influx induced by CPA or ADP. 2A-1-1 (5, 10 and 20 micromol/L) could inhibit the maximal aggregation of platelets induced by ADP with the inhibitory rates of 47.06%, 53.47% and 71.52%, respectively. 2A-1-1 at 10 and 20 micromol/L could inhibit the Ca2+ influx induced by CPA or ADP. CONCLUSIONS: 2A-1-1 can inhibit platelets aggregation, block the ROC (Receptor-dependent Ca2+ channels) and inhibit Ca2+ influx of human platelets.
Keywords:Calcium channel blockers  Platelet  Aggregation  Calciu m
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