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血小板 GP IIb-IIIa 受体拮抗剂在经皮冠状动脉介入治疗中的应用:回到未来。

Platelet GP IIb-IIIa Receptor Antagonists in Primary Angioplasty: Back to the Future.

机构信息

Division of Cardiology, "Maggiore della Carità" Hospital, Eastern Piedmont University "A. Avogadro", Novara, Italy,

出版信息

Drugs. 2015 Jul;75(11):1229-53. doi: 10.1007/s40265-015-0425-7.

Abstract

Coronary artery disease and acute myocardial infarction still represent the leading cause of mortality in developed countries. Therefore, great efforts have been made in the last decades to improve reperfusion strategies and adjunctive antithrombotic therapies. In fact, despite optimal epicardial recanalisation, a large proportion of patients still experience impaired reperfusion and in-stent thrombosis. The adjunctive use of glycoprotein (GP) IIb-IIIa inhibitors may certainly contribute in the reduction of such complications, especially when administered in the early phase of infarction. In fact, in this phase a larger platelet composition of the thrombus and the presence of a larger amount of viable myocardium, as compared to a delayed phase, may increase the benefits from this therapy and counterbalance the potential higher risk of bleeding. A large body of evidence has been accumulated on the benefits from GP IIb-IIIa inhibitors in terms of prevention of stent thrombosis, and benefits in mortality, especially among high-risk patients and as upstream strategy. Therefore, based on current available data, GP IIb-IIIa inhibitors can be recommended as early as possible (upstream strategy) among high-risk patients, such as those with advanced Killip class or anterior myocardial infarction (MI), and those presenting within the first three hours. Even though it is not universally accepted, in our opinion this strategy should be implemented in a pre-hospital setting (in ambulance) or at first hospital admission (Emergency Room or Coronary Care Unit, irrespective of whether they are in the spoke or hub hospitals). Peri-procedural intracoronary administration of GP IIb-IIIa inhibitors has not provided additional benefits as compared to intravenous administration and therefore cannot be recommended. Even though the vast majority of trials have been conducted with abciximab, several meta-analyses comparing small molecules (mainly high-dose tirofiban rather than eptifibatide) versus abciximab showed similar angiographic and clinical results between the molecules. Several recent investigations and meta-analyses have documented the higher risk of stent thrombosis associated with bivalirudin as compared to unfractionated heparin (UFH). Being that these results are independent from the use of GP IIb-IIIa inhibitors, UFH should still remain the anticoagulation therapy of choice in ST-segment elevation myocardial infarction (STEMI) patients. Minimisation of bleeding complications by extensive use of the radial approach, in the setting of STEMI, may further contribute to the adoption of a more aggressive antithrombotic and antiplatelet therapy incorporating the use of GP IIb-IIIa inhibitors. The establishment of dedicated networks for STEMI, and the large STEMI campaign, will certainly contribute to increase the proportion of patients presenting at first medical contact within the early phase (3 h) of infarction and therefore highly suitable for a more aggressive pharmacoinvasive approach with upstream administration of GP IIb-IIIa inhibitors. In fact, although the current therapeutic targets of increased rates of timely reperfusion, mainly by primary percutaneous coronary intervention (PCI), has been achieved, a deep look into the future in the fight against MI will certainly put aborting infarction as the major desirable target to be achieved.

摘要

冠状动脉疾病和急性心肌梗死仍然是发达国家死亡的主要原因。因此,在过去几十年中,人们做出了巨大努力来改善再灌注策略和辅助抗血栓治疗。事实上,尽管心外膜再通达到了最佳效果,但仍有很大一部分患者存在再灌注受损和支架内血栓形成。辅助使用糖蛋白(GP)IIb-IIIa 抑制剂肯定有助于减少这些并发症,尤其是在梗死的早期阶段使用时。事实上,在这个阶段,血栓中血小板的成分较大,存活心肌的数量也较大,与延迟阶段相比,可能会增加这种治疗的益处,并抵消潜在的更高出血风险。已经积累了大量证据表明,GP IIb-IIIa 抑制剂在预防支架内血栓形成和降低死亡率方面具有益处,尤其是在高危患者和作为上游策略时。因此,根据目前的可用数据,GP IIb-IIIa 抑制剂可以尽早(上游策略)推荐给高危患者,例如患有晚期 Killip 级或前壁心肌梗死(MI)的患者,以及在发病后的前 3 小时内出现的患者。尽管它还没有得到普遍认可,但我们认为这种策略应该在院前(在救护车上)或首次入院时(急诊室或冠心病监护病房)实施,无论他们在辐条医院还是枢纽医院。与静脉内给药相比,经皮冠状动脉内给予 GP IIb-IIIa 抑制剂并没有提供额外的益处,因此不能推荐。尽管绝大多数试验都是用阿昔单抗进行的,但几项比较小分子(主要是高剂量替罗非班,而不是依替巴肽)与阿昔单抗的荟萃分析表明,这些分子之间的血管造影和临床结果相似。最近的几项研究和荟萃分析记录了与未分级肝素(UFH)相比,比伐卢定与支架内血栓形成相关的更高风险。这些结果独立于 GP IIb-IIIa 抑制剂的使用,因此 UFH 仍然应该是 ST 段抬高型心肌梗死(STEMI)患者抗凝治疗的首选药物。在 STEMI 中广泛使用桡动脉入路来减少出血并发症,可能会进一步促进采用更积极的抗血栓和抗血小板治疗,包括使用 GP IIb-IIIa 抑制剂。STEMI 专用网络的建立和大型 STEMI 运动肯定会有助于增加在梗死早期(3 小时内)首次就诊的患者比例,因此非常适合采用更积极的药物介入治疗,上游给予 GP IIb-IIIa 抑制剂。事实上,尽管目前通过直接经皮冠状动脉介入治疗(PCI)提高及时再灌注的治疗目标已经实现,但对未来抗击心肌梗死的深入研究肯定会将中止梗死作为需要实现的主要目标。

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