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Tirofiban preserves platelet loss during continuous renal replacement therapy in a randomised prospective open-blinded pilot study

机译:替罗非班在一项连续的前瞻性随机前瞻性先导研究中,在连续肾脏替代治疗期间可保持血小板流失

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IntroductionApproximately one third of all patients with cardiogenic shock suffer from acute kidney injury. Percutaneous coronary intervention, intra-aortic balloon pump, and continuous renal replacement therapy (CRRT) require effective antiplatelet therapy and anticoagulation, resulting in a high risk for platelet loss and bleeding events. The reversible platelet glycoprotein IIb/IIIa receptor inhibitor tirofiban was investigated to preserve platelet number and activation in a prospective open-blinded endpoint evaluation study.MethodsForty patients with cardiogenic shock and acute kidney injury requiring CRRT were randomly assigned to two groups receiving unfractioned heparin (UFH) (n = 20) or a combined anticoagulation with UFH and tirofiban (n = 20). The primary endpoint was platelet loss during CRRT. Secondary endpoints were urea reduction, haemofilter life span, bleeding events, and necessity for platelet transfusions.ResultsIn UFH-treated patients, the percentage of platelet-monocyte aggregates significantly increased (P < 0.001) and consecutively platelet cell count significantly decreased (P < 0.001). In contrast, combined treatment with UFH and tirofiban significantly decreased platelet-monocyte aggregates and platelet numbers (P < 0.001).ConclusionsThis pilot study provides evidence that the use of tirofiban in addition to UFH prevents platelet loss and preserves platelet function in patients with cardiogenic shock and acute kidney injury requiring CRRT. The pathophysiological inhibition of platelet aggregation and platelet-monocyte interaction appears to be causally involved.
机译:简介所有心源性休克患者中约有三分之一患有急性肾损伤。经皮冠状动脉介入治疗,主动脉内气囊泵和持续性肾脏替代治疗(CRRT)需要有效的抗血小板治疗和抗凝治疗,导致血小板流失和出血事件的高风险。在一项前瞻性的开放式终点评估研究中,研究了可逆性血小板糖蛋白IIb / IIIa受体抑制剂替罗非班(tirofiban)来保护血小板数量和活化。方法将40例需要CRRT的心源性休克和急性肾脏损伤的患者随机分为两组,接受普通肝素(UFH) )(n = 20)或UFH和替罗非班联合抗凝治疗(n = 20)。主要终点是CRRT期间的血小板减少。次要终点是尿素减少,血液滤过器寿命,出血事件和血小板输注的必要性。结果在UFH治疗的患者中,血小板单核细胞聚集体的百分比显着增加(P <0.001),而血小板计数连续下降(P <0.001) )。相比之下,UFH和替罗非班联合治疗可显着降低血小板-单核细胞聚集和血小板数量(P <0.001)。结论这项初步研究提供了证据,证明除了UFH以外还使用替罗非班可预防心源性休克患者的血小板损失并保持血小板功能。以及需要CRRT的急性肾脏损伤。血小板聚集和血小板-单核细胞相互作用的病理生理抑制似乎是因果关系的。

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