Soluble ST2 and its relation to inflammatory, vascular atherosclerotic, and calcification markers in patients with atrial fibrillation or heart failure at moderate-to-high cardiovascular risk

Y. Yotov, Atanas Atanasov, M. Pasheva, D. Gerova, B. Galunska
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Abstract

Background: Cardiovascular diseases (CVDs) are the major cause of death globally. Among them, heart failure (HF) and atrial fibrillation (AF) result in poor prognosis and quality of life. Standard methods for assessing AF and HF, through history and physical examination, have limited sensitivity and specificity, which lead to delayed diagnosis and high risk of mortality. The identification of biomarkers able to detect the early stages of disease and/or their progression is of great importance for improving the clinical outcome. As AF and HF often coexist, it would be of great importance to find a biomarker with diagnostic utility in predicting HF in AF patients. Soluble suppression of tumorigenesis-2 (sST2) is a part of the cardioprotective IL-33/ST2 signaling pathway and may serve as a candidate biomarker for HF and AF. We aimed to evaluate sST2 serum levels in patients with AF and HF with preserved ejection fraction (HFpEF) and to explore potential relationships with traditional CVD risk factors and with novel biomarkers for vascular calcification such as undercarboxylated matrix Gla-protein (ucMGP). Materials and Methods: This study included 99 patients stratified into three groups: HFpEF (n=19), paroxysmal or persistent AF in sinus rhythm (n=33), and control group without CVD but at moderate-to-high CVD risk (n=47). Hemodynamic and anthropometric measures, coronary artery calcification (CAC), routine laboratory parameters, circulating ucMGP, and sST2 were measured. Results: sST2 levels were highly elevated in HFpEF patients. Significant positive correlation was found between sST2 and CAC-score (r=0.237, p=0.039), negative relations with serum lipids in AF patients, and positive association with serum C-reactive protein (r=0.609, p=0.018) in HFpEF patients. Soluble ST2 positively correlates with ucMGP in the entire studied population (r=0.252, p=0.006) and in the combined CVD group (AF+HFpEF) (r=0.254, p=0.036). Conclusions: sST2 levels emerge as a novel biomarker in CVD and may have prognostic importance for HF prediction in AF patients.
可溶性ST2及其与心房颤动或心力衰竭中高心血管风险患者炎症、血管粥样硬化和钙化标志物的关系
背景:心血管疾病(cvd)是全球死亡的主要原因。其中心力衰竭(HF)和心房颤动(AF)导致预后和生活质量较差。通过病史和体格检查评估房颤和心衰的标准方法灵敏度和特异性有限,导致诊断延迟和死亡率高。识别能够检测疾病早期阶段和/或其进展的生物标志物对于改善临床结果非常重要。由于房颤和心衰经常共存,寻找一种具有诊断价值的生物标志物对预测房颤患者的心衰具有重要意义。可溶性抑制肿瘤发生-2 (sST2)是心脏保护IL-33/ST2信号通路的一部分,可能作为心衰和房颤的候选生物标志物。我们旨在评估房颤和房颤患者保留射血分数(HFpEF)的血清sST2水平,并探讨其与传统心血管疾病危险因素和血管钙化的新生物标志物(如低羧化基质gla蛋白(ucMGP))的潜在关系。材料和方法:本研究纳入99例患者,分为三组:HFpEF (n=19),窦性心律阵发性或持续性房颤(n=33)和无CVD但有中高CVD风险的对照组(n=47)。测量血液动力学和人体测量、冠状动脉钙化(CAC)、常规实验室参数、循环ucMGP和sST2。结果:HFpEF患者sST2水平显著升高。sST2与cac评分呈显著正相关(r=0.237, p=0.039),与AF患者血脂呈负相关,与HFpEF患者血清c反应蛋白呈正相关(r=0.609, p=0.018)。可溶性ST2在整个研究人群(r=0.252, p=0.006)和合并CVD组(AF+HFpEF)中与ucMGP呈正相关(r=0.254, p=0.036)。结论:sST2水平作为CVD的一种新的生物标志物,可能对房颤患者的心衰预测具有重要的预后意义。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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