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首页> 外文期刊>Journal of Internal Medicine >Mon2 predicts poor outcome in ST ST ‐elevation myocardial infarction
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Mon2 predicts poor outcome in ST ST ‐elevation myocardial infarction

机译:Mon2预测ST St -Elevation心肌梗死的结果差

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Abstract Aims There are limited data on the role of human monocyte subsets in ST ‐elevation myocardial infarction ( STEMI ). The study aimed to establish the relationship between monocyte subsets, their phagocytic and nuclear factor κB ( NF κB) activity and outcomes in STEMI . Methods Monocyte subsets and their phagocytic activity and intracellular levels of inhibitory κB kinase β ( IKK β, marker of NF κB activity) were measured by flow cytometry in 245 patients with STEMI , median follow‐up of 46?months. Results Mon2 ( CD 14++ CD 16+ CCR 2+) counts were independently predictive of major adverse cardiovascular events (MACE) [4th quartile HR 3.42 (95% CI 1.43–8.16), P ?=?0.006 and 3rd quartile HR 2.88 (95% CI 1.19–7.00), P ?=?0.02 vs. 1st quartile]. Mon2 subset was the only subset associated with higher occurrence of heart failure (4th quartile vs. 1st quartile, sevenfold, P ?=?0.001 on univariate analysis; fivefold, P ?=?0.04 on multivariable analysis). On receiver operating characteristic, analysis including of Mon2 improved prognostic value of troponin T and creatine kinase for MACE and heart failure ( HF ). Higher intracellular Mon2 IKK β levels were associated with 10‐fold lower occurrence of HF on multivariable analysis (4th vs. 1st quartiles, P ?=?0.03). Abnormal Mon1 and Mon2 phagocytic capacities were related to HF development, but the association was dependent on the infarct size and other prognosticators. High Mon2 levels were associated with lower ejection fraction after STEMI onset ( P ?=?0.001) and at 6‐month follow‐up ( P ??0.001). Conclusions Abnormal Mon2 characteristics have a unique association with poor outcome in patients with STEMI . The relation of Mon2 with occurrence of HF is strongly and independently related to their functional status, which may have potential therapeutic implications.
机译:摘要目标是关于人类单核细胞亚群在ST -Elevation心肌梗死(STEMI)中的作用有限的数据。该研究旨在建立单核细胞亚群,吞噬和核因子κB(NFκB)活性和结果的关系。方法通过流式细胞仪在245例患者中,通过流式细胞术测量单核细胞亚群及其吞噬活性和细胞内抑制κB激酶β(IKKβ,NFκB活性的标志物)。结果MON2(CD14 ++ CD 16+ CCR 2+)计数独立地预测主要不良心血管事件(术术)[第4四分位数HR 3.42(95%CI 1.43-8.16),p?= 0.006和第3四宫,2.88 (95%CI 1.19-7.00),P?= 0.02与第1四分位数]。 Mon2子集是唯一与心力衰竭率较高的唯一子集(第4四分位数与第1四分位数,七倍,P?= 0.001在单变量分析上;五倍,P?= 0.04在多变量分析上)。关于接收器操作特征,分析包括MON2改善肌钙蛋白T和肌酸激酶的预后价值,用于旋转术和心力衰竭(HF)。较高的细胞内mon2 IKKβ水平与多变量分析的10倍以下的HF次数(第4次,第4四分位数,P?= 0.03)相关。异常Mon1和Mon2吞噬能力与HF发育有关,但协会依赖于梗塞大小和其他预测者。在stemi发作后(p?= 0.001)和6个月的随访后,高mon2水平与较低的喷射部分相关联(p≤≤0.001)。结论MON2特征异常具有独特的关联与Stemi患者的差异。 MON2发生的关系与HF的发生强烈,与其功能状况密切相关,其功能状况可能具有潜在的治疗含义。

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