氯吡格雷负荷剂量对择期冠状动脉支架置入患者血小板抑制的起效时间和程度：普拉格雷减少新血栓形成（PRONTO）试验

Onset and extent of platelet inhibition by clopidogrel loading in patients undergoing elective coronary stenting: the Plavix Reduction Of New Thrombus Occurrence (PRONTO) trial.

作者信息

Gurbel Paul A, Cummings Charles C, Bell Christopher R, Alford Amanda B, Meister Andrew F, Serebruany Victor L

机构信息

Sinai Center for Thrombosis Research, Sinai Hospital of Baltimore, Baltimore, MD 21215-5271, USA.

出版信息

Am Heart J. 2003 Feb;145(2):239-47. doi: 10.1067/mhj.2003.109.

DOI:10.1067/mhj.2003.109

PMID:12595840

Abstract

BACKGROUND

Despite the common practice of clopidogrel loading for coronary stenting, the time dependence and degree of platelet inhibition after this therapy are not well defined. We sought to establish an optimal clopidogrel dosing regimen for sustained platelet inhibition in stented patients.

METHODS AND RESULTS

Platelets were assessed by conventional aggregation with 5 micromol/L adenosine diphosphate (ADP), 1 microg/mL collagen (COLL), and 750 micromol/L arachidonic acid; whole blood aggregation by 1 microg/mL collagen (WBA); shear-induced closure time (CT); contractile force (CF); and expression of 9 surface receptors by flow cytometry in 100 patients undergoing elective stent placement without glycoprotein (GP) IIb/IIIa receptor antagonists. Blood was obtained at baseline and serially over 5 days poststenting after different clopidogrel loading regimens: 300 mg 24 hours before (Group A), 12 hours before (Group B), 3 to 6 hours before (Group C), and 75 mg at the time of intervention (Group D). Before stenting, ADP, COLL, CT, and WBA were reduced by clopidogrel loading (P <.05). CF was not affected by clopidogrel. Before stenting, GP IIb/IIIa expression increased in groups A through C (P <.05), whereas PECAM-1 and CD107a were reduced (P <.05). At 2 hours and 2 days poststenting, platelets, in general, exhibited an increase in activity that was most inhibited by clopidogrel loading. Clopidogrel inhibited GP Ib, platelet/endothelial cell adhesion molecule-1, CD 107a, CD 151, and GP IIb/IIIa expression at day 5 poststenting.

CONCLUSION

A 300 mg clopidogrel load given 3 to 24 hours before stenting inhibits platelets at the time of the procedure and reduces poststent activity more than a 75 mg dose given at the time of the procedure. The inhibition of adhesive molecule expression may also contribute an antithrombotic effect. Poststent activation of platelets may warrant higher periprocedural dosing.

摘要

背景

尽管冠状动脉支架置入术中普遍采用氯吡格雷负荷给药，但该治疗后血小板抑制的时间依赖性和程度尚未明确界定。我们试图为接受支架置入术的患者确定一种能持续抑制血小板的最佳氯吡格雷给药方案。

方法与结果

通过使用5微摩尔/升二磷酸腺苷（ADP）、1微克/毫升胶原（COLL）和750微摩尔/升花生四烯酸进行常规聚集试验评估血小板；通过1微克/毫升胶原进行全血聚集试验（WBA）；剪切诱导闭合时间（CT）；收缩力（CF）；以及采用流式细胞术检测100例接受择期支架置入术且未使用糖蛋白（GP）IIb/IIIa受体拮抗剂患者的9种表面受体的表达。在不同氯吡格雷负荷给药方案后，于基线及支架置入术后5天连续采集血液：术前24小时给予300毫克（A组）、术前12小时给予300毫克（B组）、术前3至6小时给予300毫克（C组）以及术中给予75毫克（D组）。在支架置入术前，氯吡格雷负荷给药可降低ADP、COLL、CT及WBA（P<.05）。CF不受氯吡格雷影响。在支架置入术前，A组至C组的GP IIb/IIIa表达增加（P<.05），而血小板内皮细胞黏附分子-1（PECAM-1）和CD107a降低（P<.05）。在支架置入术后2小时和2天，总体而言，血小板活性增加，而氯吡格雷负荷给药对此抑制作用最强。氯吡格雷在支架置入术后第5天可抑制GP Ib、血小板内皮细胞黏附分子-1、CD 107a、CD 151及GP IIb/IIIa的表达。