摘要
目的探讨普伐他汀对二磷酸腺苷(ADP)诱导的血小板PAR-1表达的影响及机制。方法体外分离富血小板血浆,分别给予C反应蛋白(CRP)、普伐他汀干预和ADP刺激进行体外研究。试验分组分别为:对照组,单纯ADP组,低浓度普代他汀+ADP组,高浓度普伐他汀组+ADP组,CRP组,普伐他汀+CRP联合组。采用流式细技术检测PAR-1和LOX-1平均荧光强度(MFI)。采用酶联免疫试验检测TXB2和F1+2水平。结果 5μmol/L ADP刺激能促使血小板PAR-1表达增加35%。50μg/mL CRP显著降低ADP诱导的血小板PAR-1的表达(P<0.01)。1μmol/L、10μmol/L普伐他汀均显著降低ADP诱导的血小板PAR-1的表达(P<0.01)。联合应用CRP和普伐他汀更能降低ADP诱导的血小板PAR-1表达,较单独使用CRP或普伐他汀降低更显著(P<0.05)。单纯ADP刺激后TXB_2较基础时明显增高(P<0.01),50μg/mL CRP、10μmol/L普伐他汀干预后ADP刺激的TXB_2分别下降为(112.68±24.48)pg/mL、(146.48±46.54)pg/mL,与单纯ADP刺激比较,差异均有统计学意义(P<0.01)。50μg/mL CRP显著增加ADP诱导的F1+2水平(P<0.01),10μmol/L普伐他汀对ADP诱导F1+2的生成无明显影响。普伐他汀呈浓度依赖性的方式降低ADP诱导的血小板LOX-1表达(1μmol/L和10μmol/L普伐他汀处理后MFI分别为:1.80±0.19和1.62±0.16),与单纯ADP刺激后LOX-1表达(MFI:3.16±0.23)比较,差异有统计学意义(P<0.01)。50μg/mL CRP对ADP刺激的血小板LOX-1表达无明显影响。结论 PAR-1在ADP诱导的血小板活化中起重要作用,普伐他汀和CRP通过不同机制明显降低ADP诱导的血小板PAR-1的表达,提示在炎症状态下他汀仍能起着重要的抗血栓作用。
Objective To study the modulation of protease-activated receptor-1(PAR-1) expression by pravastatin and C reactive protein(CRP)in vitro blood platelets.Methods Platelet-rich plasma(PRP)was isolated from peripheral blood,PRP were treated with CRP,pravastatin and ADP stimulation in vitro study.Experimental groups:blank control group,simple ADP stimulated group,low concentration of pravastatin+ADP group,high concentration pravastatin group+ADP group,CRP group,pravastatin+CRP united group.PAR-1 and LOX-1 expression on platelets were detected by flow cytometry,the result were shown by mean fluorescence intensity(MFI).TXB2 and F1+2 levels were detected by enzyme-linked immunosorbent assay.Results The 5μmol/L ADP stimulation significantly increased PAR-1expression on platelets by 35%.The 50μg/mL CRP significantly reduced platelet PAR-1 expression induced by ADP(P〈0.01).1,10μmol/L pravastatin significantly reduced platelet PAR-1expression induced by ADP(P〈0.01).Platelet PAR-1 expression induced by ADP was further reduction by combination treatment of CRP,which were significantly reduced compared with treatment of CRP or pravastatin alone(P〈0.05).Simple ADP stimulation significantly increased TXB2 level(P〈0.01).50μg/mL CRP and 10μmol/L pravastatin respectively reduced TXB2 level treated by ADP to(112.68±24.48)pg/mL and(146.48±46.54)pg/mL.Both were reduced significantly compared with ADP stimulation alone(P〈0.01).The 50μg/mL CRP significantly increased level of prothrombin fragment 1+2 induced by ADP(P〈0.01),10μmol/L pravastatin,in contrast,did not influence F1+2 level.Pravastatin reduced platelet LOX-1 expression induced by ADP in a concentration dependent manner,MFI of LOX-1on platelets treated by 1μmol/L and 10μmol/L pravastatin were 1.80±0.19 and 1.62±0.16 respectively,both were reduced significantly compared with that treated by ADP alone(MFI:3.16±0.23),P〈0.01.The 50μg/mL CRP had no significant effect on the expression of
出处
《重庆医学》
CAS
北大核心
2016年第11期1459-1462,共4页
Chongqing medicine
基金
国家自然科学基金资助项目(81160030)
