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首页> 外文期刊>Cardiovascular therapeutics >Bivalirudin Inhibits Periprocedural Platelet Function and Tissue Factor Expression of Human Smooth Muscle Cells
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Bivalirudin Inhibits Periprocedural Platelet Function and Tissue Factor Expression of Human Smooth Muscle Cells

机译:比伐卢定抑制人平滑肌细胞的围手术期血小板功能和组织因子表达

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摘要

Aim: A major concern of stent implantation after percutaneous coronary intervention (PCI) is acute stent thrombosis. Effective inhibition of periprocedural platelet function in patients with coronary artery disease (CAD) leads to an improved outcome. In this study, we examined the periprocedural platelet reactivity after administrating bivalirudin during PCI compared to unfractionated heparin (UFH) administration. Further, the effect of bivalirudin on induced tissue factor (TF) expression in smooth muscle cells (SMC) was determined. Methods: Patients with CAD (n = 58) and double antithrombotic medication were treated intraprocedural with UFH (n = 30) or bivalirudin (n = 28). Platelet activation markers were flow cytometrically measured before and after stenting. The expression of TF in SMC was determined by real-time PCR and Western blotting. The thrombogenicity of platelet-derived microparticles and SMC was assessed via a TF activity assay. Results: Bivalirudin significantly diminished the agonist-induced platelet reactivity post-PCI. Compared to UFH treatment, the adenosine diphosphate (ADP) and thrombin receptor-activating peptide (TRAP)-induced thrombospondin expression post-PCI was reduced when bivalirudin was administrated during intervention. In contrast to UFH, bivalirudin reduced the P-selectin expression of unstimulated and ADP-induced platelets post-PCI. Moreover, bivalirudin inhibited the thrombin-, but not FVIIa- or FVIIa/FX-induced TF expression and pro-coagulant TF activity of SMC. Moreover, bivalirudin reduced the TF activity of platelet-derived microparticles postinduction with TRAP or ADP. Conclusions: Bivalirudin is better than UFH in reducing periprocedural platelet activation. Moreover, thrombin-induced TF expression is inhibited by bivalirudin. Thus, bivalirudin seems to be a better anticoagulant during PCI than UFH.
机译:目的:经皮冠状动脉介入治疗(PCI)后支架植入的主要问题是急性支架血栓形成。有效抑制冠心病(CAD)患者的术中血小板功能可改善预后。在这项研究中,我们检查了与普通肝素(UFH)相比,PCI期间比伐卢定给药后过程性血小板反应性。此外,确定了比伐卢定对平滑肌细胞(SMC)中诱导的组织因子(TF)表达的影响。方法:CAD(n = 58)和双重抗栓药物的患者在手术过程中用UFH(n = 30)或bivalirudin(n = 28)治疗。在置入支架之前和之后,通过流式细胞仪测量血小板活化标志物。实时荧光定量PCR和Western blotting检测TF在SMC中的表达。通过TF活性测定评估血小板衍生的微粒和SMC的血栓形成性。结果:比伐卢定显着降低PCI后激动剂诱导的血小板反应性。与UFH治疗相比,在干预期间给予比伐卢定时,PCI后腺苷二磷酸(ADP)和凝血酶受体激活肽(TRAP)诱导的血小板反应蛋白表达降低。与UFH相反,比伐卢定可降低PCI后未刺激和ADP诱导的血小板的P选择素表达。此外,比伐卢定抑制凝血酶,但不抑制FVIIa-或FVIIa / FX诱导的SMC的TF表达和促凝血TF活性。此外,比伐卢定降低了TRAP或ADP诱导后血小板衍生的微粒的TF活性。结论:比伐卢定在减少围手术期血小板活化方面优于UFH。此外,比伐卢定抑制凝血酶诱导的TF表达。因此,比伐卢定似乎比UFH在PCI期间具有更好的抗凝作用。

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