首页> 外文期刊>Clinical and Experimental Immunology: An Official Journal of the British Society for Immunology >Circulating lectin pathway proteins do not predict short‐term cardiac outcomes after myocardial infarction
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Circulating lectin pathway proteins do not predict short‐term cardiac outcomes after myocardial infarction

机译:循环凝集素途径蛋白质不会预测心肌梗死后的短期心脏结果

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Summary Despite improvements in treatment, coronary artery disease is still responsible for one‐third of all deaths globally, due predominantly to myocardial infarction (MI) and stroke. There is an important potential in developing new strategies for treatment of patients with these conditions. Inflammation, and in particular the actions of the complement system, has emerged as part of the pathogenesis in reperfusion injury in patients with MI. To further qualify this, we examined the association between the plasma levels of lectin pathway proteins and myocardial end‐points, left ventricular ejection fraction (LVEF) and infarct size in a cohort of patients with ST‐elevation myocardial infarction (STEMI). A blood sample was drawn the day after percutaneous coronary intervention from 73 patients with STEMI. The primary end‐points, LVEF and infarct size, were measured with magnetic resonance imaging 6–9?days after the infarct. Complement pattern‐recognition molecules of the lectin pathway (mannan‐binding lectin, H‐ficolin, L‐ficolin and M‐ficolin) were analysed along with soluble membrane attack complex (sMAC) and C‐reactive protein (CRP) in plasma with immunofluorometric assays 50%. CRP correlated negatively with LVEF, regression coefficient?=?–0·17 ( P ?=?0·01). None of the lectin pathway proteins correlated to LVEF or infarct size, nor did soluble membrane attack complex (sMAC). There were no differences in plasma levels of these complement proteins when comparing patients with ejection fraction 50% to patients with ejection fraction 50%. Pattern‐recognition molecules of the lectin pathway and sMAC do not predict short‐term cardiac outcomes after MI.
机译:发明虽然治疗有所改善,但冠状动脉疾病仍然负责全球所有死亡的三分之一,主要是由于心肌梗塞(MI)和中风。开发患有这些条件患者的新策略具有重要潜力。炎症,特别是补体系统的作用,作为MI患者再灌注损伤的病机的一部分。为了进一步符合权利要求,我们研究了凝集素途径蛋白和心肌终点,左心室喷射分数(LVEF)和梗塞队的血浆末端,梗塞群体之间的关联,在ST升高的心肌梗死患者(Stemi)中。从73例干药患者经皮冠状动脉介入后的一天绘制了血液样本。初级终点,LVEF和梗塞尺寸用磁共振成像6-9?梗塞后的天数。通过免疫荧光测定仪和血浆中的可溶性膜攻击复合物(SMAC)和C反应蛋白(CRP)分析凝集素途径(甘露甘油结合凝集素,H-Ficolin,L- Ficolin和M-Ficolin)的补体模式识别分子。测定& 50%。 CRP与LVEF,回归系数呈负相关,回归系数?=? - 0·17(p?=?0·01)。没有凝集素途径蛋白质与LVEF或梗塞尺寸相关,也不是可溶性膜攻击复合物(SMAC)。当将射血分数的患者与射血分数的患者比较时,这些补体蛋白的血浆水平没有差异。凝集素途径和SMAC的图案识别分子不会预测MI后的短期心脏结果。

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