基于动态S100A8/A9水平的急性冠状动脉综合征后心力衰竭风险分层的开发与验证

Development and Validation of Risk Stratification for Heart Failure After Acute Coronary Syndrome Based on Dynamic S100A8/A9 Levels.

作者信息

Ma Jie, Ma Ke, Chen Jing, Yang Xinying, Gao Fei, Gao Hai, Zhang Hui, Ma Xin-Liang, Du Jie, Li Ping, Li Yulin

机构信息

Beijing Anzhen Hospital of Capital Medical University Beijing China.

Beijing Institute of Heart Lung and Blood Vessel Diseases Beijing China.

出版信息

J Am Heart Assoc. 2025 Feb 4;14(3):e037401. doi: 10.1161/JAHA.124.037401. Epub 2025 Feb 3.

DOI:10.1161/JAHA.124.037401

PMID:39895550

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12074705/

Abstract

BACKGROUND

The early assessment of heart failure (HF) risk in patients with acute coronary syndrome (ACS) can help reduce mortality. S100A8/A9 is not only rapidly released after myocardial ischemia, but is also involved in reperfusion injury, which is an important predictor of HF after ACS. We attempted to construct a reliable HF risk stratification tool for evaluating patients with ACS after reperfusion therapy based on S100A8/A9 dynamic changes.

METHODS AND RESULTS

This prospective study included 3 independent cohorts of patients with ACS who received reperfusion therapy. The discovery cohort was divided into 2 subgroups: the longitudinal subgroup (n=264) with serum S100A8/A9 levels measured at admission and on days 1, 2, 3, and 4 postadmission, respectively, and the 2-point subgroup (n=798) with S100A8/A9 levels measured at admission and on day 1 postadmission, respectively. Validation cohorts 1 (n=1399) and 2 (n=1183) both had S100A8/A9 levels measured on day 1 postadmission. HF events included in-hospital HF events after the initial presentation and long-term HF events after discharge. The median follow-up for the discovery cohort, validation cohort 1, and validation cohort 2 was 4.2, 2.6, and 1.8 years, respectively. In the discovery cohort, S100A8/A9's predictive ability at day 1 surpassed other time points. Through the S100A8/A9-guided risk stratification, patients deemed high risk (>7900 ng/mL) exhibited a higher 1-year HF event rate (46% versus 2%, 38% versus 5%) than patients at low risk (<2100 ng/mL) in both validation cohorts. Among patients without left ventricular dysfunction after ACS, β-blocker therapy correlated with reduced 1-year HF events in intermediate-to- high-risk patients but not in low-risk patients.

CONCLUSIONS

S100A8/A9 levels on day 1 accurately classified patients at varying risks of HF, serving as a robust tool for HF risk prediction and treatment guidance.

REGISTRATION

URL: https://www.clinicaltrials.gov; Unique identifier: NCT03752515.

摘要

背景

急性冠状动脉综合征（ACS）患者心力衰竭（HF）风险的早期评估有助于降低死亡率。S100A8/A9不仅在心肌缺血后迅速释放，还参与再灌注损伤，是ACS后HF的重要预测指标。我们试图基于S100A8/A9的动态变化构建一种可靠的HF风险分层工具，用于评估接受再灌注治疗的ACS患者。

方法与结果

这项前瞻性研究纳入了3个接受再灌注治疗的ACS患者独立队列。发现队列分为2个亚组：纵向亚组（n = 264），分别在入院时以及入院后第1、2、3和4天测量血清S100A8/A9水平；两点亚组（n = 798），分别在入院时和入院后第1天测量S100A8/A9水平。验证队列1（n = 1399）和验证队列2（n = 1183）均在入院后第1天测量S100A8/A9水平。HF事件包括首次就诊后的院内HF事件和出院后的长期HF事件。发现队列、验证队列1和验证队列2的中位随访时间分别为4.2年、2.6年和1.8年。在发现队列中，S100A8/A9在第1天的预测能力超过其他时间点。通过S100A8/A9指导的风险分层，在两个验证队列中，被判定为高风险（>7900 ng/mL）的患者1年HF事件发生率高于低风险（<2100 ng/mL）患者（46%对2%，38%对5%）。在ACS后无左心室功能障碍的患者中，β受体阻滞剂治疗与中高危患者1年HF事件减少相关，但与低风险患者无关。