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Relationship of IgG and IgM autoantibodies and immune complexes to oxidized LDL with markers of oxidation and inflammation and cardiovascular events: results from the EPIC-Norfolk Study

机译:IgG和IgM自身抗体免疫复合物与氧化的LDL的关系以及氧化炎症和心血管事件的标志物:EPIC-Norfolk研究的结果

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摘要

Levels of IgG and IgM autoantibodies (AA) to malondialdehyde (MDA)-LDL and apoB-immune complexes (ICs) were measured in 748 cases and 1,723 controls in the EPIC-Norfolk cohort and their association to coronary artery disease (CAD) events determined. We evaluated whether AA and IC modify CAD risk associated with secretory phospholipase A2 (sPLA2) type IIA mass and activity, lipoprotein-associated PLA2 activity, lipoprotein (a) [Lp(a)], oxidized phospholipids on apoB-100 (OxPL/apoB), myeloperoxidase, and high sensitivity C-reactive protein. IgG ICs were higher in cases versus controls (P = 0.02). Elevated levels of IgM AA and IC were inversely associated with Framingham Risk Score and number of metabolic syndrome criteria (p range 0.02–0.001). In regression analyses adjusted for age, smoking, diabetes, LDL-cholesterol, HDL-cholesterol, and systolic blood pressure, the highest tertiles of IgG and IgM AA and IC were not associated with higher risk of CAD events compared with the lowest tertiles. However, elevated levels of IgM IC reduced the risk of Lp(a) (P = 0.006) and elevated IgG MDA-LDL potentiated the risk of sPLA2 mass (P = 0.018). This epidemiological cohort of initially healthy subjects shows that IgG and IgM AA and IC are not independent predictors of CAD events but may modify CAD risk associated with elevated levels of oxidative biomarkers.
机译:在EPIC-诺福克队列中的748例和1,723例对照中测量了针对丙二醛(MDA)-LDL和apoB免疫复合物(IC)的IgG和IgM自身抗体(AA)的水平,并确定了它们与冠心病(CAD)事件的相关性。我们评估了AA和IC是否会改变与IIA型分泌性磷脂酶A2(sPLA2)的质量和活性,脂蛋白相关的PLA2活性,脂蛋白(a)[Lp(a)],载脂蛋白100(OxPL / apoB上的氧化磷脂)相关的CAD风险),髓过氧化物酶和高灵敏度C反应蛋白。与对照组相比,IgG ICs更高(P = 0.02)。 IgM AA和IC的升高与Framingham风险评分和代谢综合征标准数呈负相关(p范围0.02–0.001)。在对年龄,吸烟,糖尿病,LDL-胆固醇,HDL-胆固醇和收缩压进行校正的回归分析中,与最低的三分位数相比,IgG和IgM AA和IC的最高三分位数与较高的CAD事件风险无关。但是,升高的IgM IC降低了Lp(a)的风险(P = 0.006),而升高的IgG MDA-LDL则增加了sPLA2质量的风险(P = 0.018)。最初健康受试者的这一流行病学队列显示,IgG,IgMAA和IC并不是CAD事件的独立预测因子,但可能会改变与氧化生物标志物水平升高相关的CAD风险。

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