首页> 外文期刊>Heart >Plasma von Willebrand factor, soluble thrombomodulin, and fibrin D-dimer concentrations in acute onset non-rheumatic atrial fibrillation.
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Plasma von Willebrand factor, soluble thrombomodulin, and fibrin D-dimer concentrations in acute onset non-rheumatic atrial fibrillation.

机译:急性发作性非风湿性心房颤动的血浆von Willebrand因子,可溶性血栓调节蛋白和纤维蛋白D-二聚体浓度。

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OBJECTIVE: To investigate whether new onset acute atrial fibrillation (AF) of < 48 hours' duration creates a prothrombotic state in the absence of anticoagulation and to assess the evolution in research indices after spontaneous or pharmacological cardioversion. METHODS: 24 patients were recruited with first onset acute non-rheumatic AF, in whom sinus rhythm was restored within 48 hours of arrhythmia onset, without anticoagulant treatment. Atrial mechanical function was assessed by transmitral inflow. Soluble thrombomodulin and von Willebrand factor concentrations (both as indices of endothelial damage or dysfunction) and fibrin D-dimer concentrations (as an index of thrombogenesis) were measured. Blood samples were drawn and echocardiographic studies were performed at days 1, 3, 7, and 30 after cardioversion. Research indices were compared with those of 24 healthy participants, 24 patients with chronic AF, and 24 patients with ischaemic heart disease in sinus rhythm. RESULTS: Patients with AF had higher concentrations of soluble thrombomodulin (acute AF 12.1 (4.1) ng/ml; chronic AF 11.8 (4.6) ng/ml), von Willebrand factor (acute AF 137.2 (36.9) ng/ml; chronic AF 133.1 (25.0) ng/ml), and fibrin D-dimer concentrations (acute AF 2.35 (2.68) microg/ml; chronic AF 1.12 (0.65) microg/ml) than did healthy controls (5.9 (2.7) ng/ml, 86.7 (33.2) ng/ml, and 0.39 (0.28) microg/ml, respectively) and patients with ischaemic heart disease (7.4 (3.7) ng/ml, 110.0 (29.0) ng/ml, and 0.99 (0.73) microg/ml, respectively) (all p < 0.05). Day 30 concentrations of fibrin D-dimer were higher in patients with acute AF than in patients with chronic AF (p = 0.038) but sTM and von Willebrand factor concentrations were not different (both not significant). There were no significant changes in research indices or echocardiographic parameters after cardioversion (all p > 0.05). CONCLUSIONS: There was evidence among patients with acute onset AF of endothelial damage or dysfunction and increased thrombogenesis, which persisted up to30 days after cardioversion.
机译:目的:研究持续时间少于48小时的新发急性心房颤动(AF)是否在没有抗凝治疗的情况下形成血栓形成状态,并评估自发或药理性心脏复律后研究指标的变化。方法:招募了24例首次发作的急性非风湿性AF患者,其在心律不齐发作后48小时内恢复了窦性心律,未进行抗凝治疗。心房机械功能通过经皮入流评估。测量了可溶性血栓调节蛋白和von Willebrand因子浓度(均作为内皮损伤或功能障碍的指标)和血纤蛋白D-二聚体浓度(作为血栓形成的指标)。在心脏复律后第1、3、7和30天抽取血样并进行超声心动图研究。将研究指标与24名健康参与者,24名慢性房颤患者和24名缺血性心脏病患者的窦律进行比较。结果:AF患者的可溶性血栓调节蛋白浓度更高(急性AF 12.1(4.1)ng / ml;慢性AF 11.8(4.6)ng / ml),von Willebrand因子(急性AF 137.2(36.9)ng / ml;慢性AF 133.1 (25.0)ng / ml)和纤维蛋白D-二聚体浓度(急性AF 2.35(2.68)microg / ml;慢性AF 1.12(0.65)microg / ml)比健康对照组(5.9(2.7)ng / ml,86.7(分别为33.2)ng / ml和0.39(0.28)microg / ml)和缺血性心脏病患者(分别为7.4(3.7)ng / ml,110.0(29.0)ng / ml和0.99(0.73)microg / ml) )(所有p <0.05)。急性房颤患者第30天的血纤蛋白D-二聚体浓度高于慢性房颤患者(p = 0.038),但sTM和von Willebrand因子浓度无差异(均无统计学意义)。复律后研究指标或超声心动图参数无明显变化(所有p> 0.05)。结论:在急性发作性房颤患者中有证据表明内皮损害或功能障碍和血栓形成增加,这种现象在心脏复律后持续了30天。

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