Effects of low-molecular-weight heparin treatment on fibrinolytic markers in unstable coronary artery disease

H. Toss , L. Wallentin , A. Siegbahn
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引用次数: 1

Abstract

Abstract Objectives : Low-molecular-weight heparins (LMWHs) efficiently reduce the coagulant activity, but their influence on the fibrinolytic system and fibrin turnover is not fully elucidated. We therefore determined markers offibrinolytic activity, fibrin turnover and inflammation in LMWH treated patients with acute coronary artery disease. Design : Double-blind placebo controlled clinical trial. Setting : Consecutive patients admitted at two centers. Subjects : Individuals with unstable angina or non-Q-wave MI ( n = 87). Interventions : Randomized to placebo-controlled subcutaneous dalteparin treatment, 120 IU/kg bw twice daily for 5–8 days and 7500IU once daily over the next 35–45 days. Main outcome measures : Markers of fibrinolytic activity, i.e. tissue plasminogen activator (t-PA) antigen, plasminogen activator inhibitor 1 (PAI-1) activity, plasminogen anti-plasmin (PAP) complex, and D-dimer determined at inclusion, after 2, 5 and 40–50 days. C-reactive protein (CRP), fibrinogen and prothrombin fragment 1+2 (F1+2) were determined at inclusion. Results : At inclusion there were positive correlations between fibrinogen, CRP and D-dimer levels. During LMWH treatment there was a marked increase in t-PA antigen concentration, a rise in PAI-1 activity and a slight decrease in PAP-complex levels. The LMWH administration was also associated with a long-lasting decrease in the D-dimer concentrations. In the placebo group there was a slight and transient increase in all the evaluated markers of fibrinolytic activity and fibrin turnover. Conclusion : In unstable CAD increased inflammatory activity is associated with increased thrombin generation and fibrin turnover. During LMWH treatment there is a sustained reduction in fibrin turnover and no rise in plasmin generation despite an increase in t-PA level.
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低分子肝素治疗对不稳定冠状动脉疾病患者纤溶标志物的影响
目的:低分子肝素(LMWHs)有效降低凝血活性,但其对纤溶系统和纤维蛋白周转的影响尚未完全阐明。因此,我们确定了低分子肝素治疗的急性冠状动脉疾病患者的纤维蛋白溶解活性、纤维蛋白周转和炎症标志物。设计:双盲安慰剂对照临床试验。设置:两个中心连续收治患者。受试者:患有不稳定型心绞痛或非Q波MI的个体(n=87)。干预措施:随机接受安慰剂对照皮下达肝素治疗,120 IU/kg bw,每天两次,持续5-8天,7500IU,在接下来的35-45天每天一次。主要结果指标:纤溶活性的标志物,即组织纤溶酶原激活物(t-PA)抗原、纤溶酶原激活剂抑制剂1(PAI-1)活性、纤溶酶原-抗纤溶酶(PAP)复合物和D-二聚体,在纳入时、2、5和40-50天后测定。纳入时测定C反应蛋白(CRP)、纤维蛋白原和凝血酶原片段1+2(F1+2)。结果:纤维蛋白原、C反应蛋白和D-二聚体水平在纳入时呈正相关。在LMWH治疗期间,t-PA抗原浓度显著增加,PAI-1活性升高,PAP复合物水平略有下降。低分子肝素给药也与D-二聚体浓度的长期下降有关。在安慰剂组中,所有评估的纤溶活性和纤维蛋白周转的标志物都有轻微和短暂的增加。结论:在不稳定型CAD中,炎症活性的增加与凝血酶生成和纤维蛋白周转的增加有关。在低分子肝素治疗期间,尽管t-PA水平增加,但纤维蛋白周转持续减少,纤溶酶生成没有增加。
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Editorial Impaired liver regeneration after partial hepatectomy in plasminogen deficient mice Covariance of metabolic and hemostatic risk indicators in men and women Endogeneous fibrinolysis and restenosis of peripheral arteries after percutaneous transluminal angioplasty Effects of low-molecular-weight heparin treatment on fibrinolytic markers in unstable coronary artery disease
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