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首页> 外文期刊>Journal of cardiovascular translational research >Measurement of novel biomarkers to predict chronic heart failure outcomes and left ventricular remodeling
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Measurement of novel biomarkers to predict chronic heart failure outcomes and left ventricular remodeling

机译:测量新型生物标志物以预测慢性心力衰竭结果和左心室重塑

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摘要

Myocardial remodeling is pivotal in the progression and complication of chronic heart failure (HF). We assessed serial measurement of five biomarkers with biologic links to remodeling (biglycan, secreted frizzled-related protein 3, endostatin, insulin-like growth factor binding protein 7 IGFBP7, mimecan) in 142 patients with HF followed through 882 office visits. IGFBP7 and mimecan were most associated with events; in fully adjusted models, lower IGFBP7 concentrations across visits independently predicted fewer events (odds ratio OR=0.83; 95 confidence interval CI=0.73-0.95, p=0.01). Subjects with rising mimecan had greater decrease in left ventricular end diastolic (p=0.07) and systolic (p=0.01) volumes, greater increase in ejection fraction (p=0.02), and had lowest event rates. Statistical models suggested several HF medications might lead to changes in both IGFBP7 and mimecan values. The results suggest serial measurement of IGFBP7 provides prognostic information, while changes in mimecan provide unique information regarding myocardial remodeling.
机译:心肌重塑在慢性心力衰竭 (HF) 的进展和并发症中起着关键作用。我们评估了 142 名 HF 患者对 882 次就诊的 5 种与重塑有生物学联系的生物标志物(biglycan、分泌型卷曲相关蛋白 3、内皮抑素、胰岛素样生长因子结合蛋白 7 [IGFBP7]、mimecan)的连续测量。IGFBP7 和 mimecan 与事件最相关;在完全调整的模型中,两次就诊时较低的IGFBP7浓度独立预测的事件较少(比值比[OR]=0.83;95%置信区间[CI]=0.73-0.95,p=0.01)。mimecan 升高的受试者左心室舒张末期 (p=0.07) 和收缩期 (p=0.01) 容积减少较大,射血分数增加较多 (p=0.02),事件发生率最低。统计模型表明,几种 HF 药物可能导致 IGFBP7 和 mimecan 值的变化。结果表明,IGFBP7的连续测量提供了预后信息,而mimecan的变化提供了有关心肌重塑的独特信息。

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