Atherogenesis is a complex inflammatory process stemming from the accumulation and oxidation of low density lipoproteins (LDL). IgM autoantibodies against phosphorylcholine (anti-PC) bind to the PC epitope on oxidized LDL (OxLDL), inhibiting the uptake of oxLDL by macrophages in atherosclerotic lesions. Anti-PC autoantibodies have been reported to be protective against atherothrombosis. We investigated the relationship of anti-PC concentrations with cardiovascular outcomes in patients with acute coronary syndromes (ACS). We measured anti-PC levels within 7 days of an ACS in 3,356 patients enrolled in the ATLAS ACS-TIMI 46 trial, a randomized dose ranging study of rivaroxaban versus placebo. The primary endpoint was death, myocardial infarction (MI), stroke, or severe recurrent ischemia (SRI) requiring revascularization during 6 months. The median baseline anti-PC concentration was 40.9 U/mL (25th, 75th percentiles: 25.4, 67.4). There was no significant association between anti-PC levels and the primary endpoint (Q1: 6.8 %, Q2: 4.2 %, Q3: 7.8 %, Q4: 5.4 %, p-trend = 0.87), all-cause mortality (Q1: 1.4 %, Q2: 0.7 %, Q3: 2.4 %, Q4: 0.9 %, p-trend = 0. 96), or any of the other individual endpoint components (MI: p-trend = 0.87, Stroke: p-trend = 0.43, SRI: p-trend = 0.66). Using the previously reported anti-PC cutpoint of 17 U/mL did not reveal a significant relationship between anti-PC concentrations and cardiovascular outcomes (<17 U/mL: 8.1 % vs. ≥17 U/mL: 5.8 %; p = 0.11). Similarly, evaluation of anti-PC as a continuous variable did not reveal a significant association (p = 0.30). In this study of patients early after ACS undergoing intensive secondary preventive therapy, IgM anti-PC titers did not exhibit a significant relationship with cardiovascular outcomes.

译文

动脉粥样硬化是一个复杂的炎症过程,源于低密度脂蛋白 (LDL) 的积累和氧化。针对磷酸胆碱的IgM自身抗体 (抗PC) 与氧化LDL (OxLDL) 上的PC表位结合,从而抑制动脉粥样硬化病变中巨噬细胞对oxLDL的摄取。据报道,抗PC自身抗体可预防动脉粥样硬化血栓形成。我们研究了急性冠脉综合征 (ACS) 患者抗PC浓度与心血管结局的关系。我们在参加ATLAS ACS-TIMI 46试验的3,356名患者中测量了ACS 7天内的抗PC水平,该试验是利伐沙班与安慰剂的随机剂量范围研究。主要终点是死亡,心肌梗死 (MI),中风或需要在6个月内进行血运重建的严重复发性缺血 (SRI)。基线抗PC浓度中位数为40.9 U/mL (第25,75个百分位数: 25.4,67.4)。抗PC水平与主要终点 (Q1: 6.8%,Q2: 4.2%,Q3: 7.8%,Q4: 5.4%,p-趋势 = 0.87),全因死亡率 (Q1: 1.4%,Q2: 0.7%,Q3: 2.4%,Q4: 0.9%,p-趋势 = 0.96),或任何其他单独的终点分量 (MI: p-趋势 = 0.87,冲程: p-趋势 = 0.43,SRI: p-趋势 = 0.66)。使用先前报道的17 u/mL的抗PC切点未揭示抗PC浓度与心血管结局之间的显着关系 (<17 u/mL: 8.1% vs. ≥ 17 u/mL: 5.8%; p = 0.11)。类似地,作为连续变量的抗PC评价没有显示出显著的关联 (p = 0.30)。在这项研究中,ACS接受强化二级预防治疗后的早期患者,IgM抗PC滴度与心血管结局没有显着关系。

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