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早期支架血栓形成史与血栓溶解时间延长有关。

A history of early stent thrombosis is associated with prolonged clot lysis time.

机构信息

John Paul II Hospital, Krakow, Poland.

出版信息

Thromb Haemost. 2012 Mar;107(3):513-20. doi: 10.1160/TH11-09-0662. Epub 2012 Jan 25.

DOI:10.1160/TH11-09-0662
PMID:22274545
Abstract

It has been demonstrated that formation of compact plasma fibrin clots resistant to plasmin-mediated lysis characterises patients following in-stent thrombosis (IST). The relationship between defective fibrinolysis, reflected as prolonged clot lysis time (CLT) and IST is unclear. We sought to investigate whether patients with acute and subacute IST have impaired fibrinolytic capacity. We studied 41 definite IST patients, including 15 with acute and 26 with subacute IST experienced 2-73 months prior to enrollment, versus 41 controls matched for demographics, cardiovascular risk factors, concomitant treatment and angiographic/stent parameters. CLT, reflecting lysis of a tissue factor-induced plasma clot by exogenous tissue plasminogen activator, together with plasminogen activator inhibitor-1 (PAI-1) antigen and activity, thrombin-activatable fibrinolysis inhibitor (TAFI) antigen and activity, thrombomodulin (TM), plasminogen and α2-antiplasmin (α2AP) were measured. There were no inter-group differences in angiographic parameters, indication to the first PCI, culprit vessel or a type of stent. Patients with IST had 11% longer CLT (p=0.005) and 13% higher PAI-1 antigen (p=0.04) compared to controls. There were positive correlations in both groups between CLT and PAI-1 antigen and TAFI activity (all p<0.001). Multiple regression analysis showed that CLT (odds ratio [OR]=1.04 per 1 minute, 95% CI 1.01-1.08, p=0.02) and platelet count (OR=1.01 per 1,000/μl, 95% CI 1.00-1.02, p=0.034) were independent predictors of IST (R(2)=0.28, p<0.05). Concluding, impaired fibrinolytic potential, that is in part determined by plasma PAI-1 antigen and TAFI activity, characterises patients with a history of acute and subacute IST, which might help identify patients at higher risk of IST.

摘要

已经证明,抵抗纤溶酶介导的溶解的致密血浆纤维蛋白凝块的形成是支架内血栓形成(IST)后的患者的特征。纤溶缺陷与 IST 的关系,表现为凝血块溶解时间(CLT)延长,尚不清楚。我们试图研究急性和亚急性 IST 患者是否存在纤溶能力受损。我们研究了 41 例明确的 IST 患者,包括 15 例急性 IST 和 26 例亚急性 IST,这些患者在入组前 2-73 个月发生 IST,与 41 例在人口统计学、心血管危险因素、伴随治疗和血管造影/支架参数方面相匹配的对照组进行比较。CLT 反映了外源性组织纤溶酶原激活物对组织因子诱导的血浆凝块的溶解,同时还测量了纤溶酶原激活物抑制剂-1(PAI-1)抗原和活性、凝血酶激活的纤溶抑制物(TAFI)抗原和活性、血栓调节蛋白(TM)、纤溶酶原和α2-抗纤溶酶(α2AP)。两组之间的血管造影参数、首次 PCI 的适应证、罪犯血管或支架类型均无差异。与对照组相比,IST 患者的 CLT 长 11%(p=0.005),PAI-1 抗原高 13%(p=0.04)。两组中 CLT 与 PAI-1 抗原和 TAFI 活性均呈正相关(均 p<0.001)。多元回归分析显示,CLT(优势比[OR]=每增加 1 分钟 1.04,95%置信区间 1.01-1.08,p=0.02)和血小板计数(OR=每增加 1,000/μl 1.01,95%置信区间 1.00-1.02,p=0.034)是 IST 的独立预测因素(R(2)=0.28,p<0.05)。总之,纤溶能力受损,部分由血浆 PAI-1 抗原和 TAFI 活性决定,其特征是急性和亚急性 IST 后的患者,这可能有助于识别 IST 风险较高的患者。

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