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血小板PAR1受体密度——与血小板活化反应及血小板活化后暴露变化的相关性

Platelet PAR1 receptor density--correlation to platelet activation response and changes in exposure after platelet activation.

作者信息

Ramström Sofia, Oberg Karin Vretenbrant, Akerström Finn, Enström Camilla, Lindahl Tomas L

机构信息

Department of Biomedicine and Surgery, Division of Clinical Chemistry, University Hospital, SE-581 85 Linköping, Sweden.

出版信息

Thromb Res. 2008;121(5):681-8. doi: 10.1016/j.thromres.2007.06.010. Epub 2007 Aug 1.

Abstract

INTRODUCTION

A polymorphism (-14 A/T) affecting PAR1 expression on the platelet surface has recently been identified. A two-fold variation in receptor density, which correlated with the platelet response to PAR1-activating peptide (PAR1-AP), has been reported.

MATERIALS AND METHODS

We used flow cytometry to measure the correlation between the number of PAR1 receptors and platelet activation. We also measured the changes in receptor exposure after platelet activation with PAR1-AP, ADP, PAR4-AP or a collagen-related peptide (CRP).

RESULTS

In our study, the PAR1 receptor number varied almost four-fold, from 547 to 2063 copies/platelet (mean+/-S.D. 1276+/-320, n=70). The number of PAR1 receptors on resting platelets correlated to platelet fibrinogen binding and P-selectin expression following platelet activation with PAR1-AP (r(2)=0.30, p<0.01 and r(2)=0.15, p<0.05, respectively, n=36). The correlation was not improved by exclusion of the ADP-component from the PAR1-AP-induced response. We found a trend, but no statistically significant differences in PAR1 receptor number and platelet reactivity between A/A individuals and T/A or T/T individuals. Ex vivo activation with PAR1-AP decreased PAR1 surface exposure to 71+/-19% of the exposure on resting platelets (mean+/-S.D., p<0.01, n=19), while activation by ADP, PAR4-AP or CRP significantly increased the exposure, to 151+/-27%, 120+/-21% and 138+/-25%, respectively (n=11, 11 and 10).

CONCLUSIONS

This study shows a large variation in PAR1 receptor number in healthy individuals, a variation correlated to the platelet activation response. We found a significant reduction in PAR1 surface exposure after adding PAR1-AP, while activation with ADP, PAR4-AP or CRP increased the exposure.

摘要

引言

最近发现一种影响血小板表面PAR1表达的多态性(-14 A/T)。据报道,受体密度存在两倍的差异,这与血小板对PAR1激活肽(PAR1-AP)的反应相关。

材料与方法

我们使用流式细胞术测量PAR1受体数量与血小板活化之间的相关性。我们还测量了用PAR1-AP、ADP、PAR4-AP或胶原相关肽(CRP)激活血小板后受体暴露的变化。

结果

在我们的研究中,PAR1受体数量变化近四倍,从547个/血小板到2063个/血小板(平均值±标准差1276±320,n = 70)。静息血小板上PAR1受体的数量与用PAR1-AP激活血小板后血小板纤维蛋白原结合和P-选择素表达相关(r² = 0.30,p < 0.01和r² = 0.15,p < 0.05,n = 36)。从PAR1-AP诱导的反应中排除ADP成分后,相关性并未改善。我们发现A/A个体与T/A或T/T个体之间在PAR1受体数量和血小板反应性方面有趋势但无统计学显著差异。用PAR1-AP进行体外激活使PAR1表面暴露减少至静息血小板暴露的71±19%(平均值±标准差,p < 0.01,n = 19),而用ADP、PAR4-AP或CRP激活则使暴露显著增加,分别为151±27%、120±21%和138±25%(n = 11、11和10)。

结论

本研究表明健康个体中PAR1受体数量存在很大差异,这种差异与血小板活化反应相关。我们发现添加PAR1-AP后PAR1表面暴露显著减少,而用ADP、PAR4-AP或CRP激活则增加了暴露。

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