Proteomics Identify Clinical Phenotypes and Predict Functional Outcomes in Heart Failure With Preserved Ejection Fraction: Insights From VITALITY-HFpEF.

IF 7.8 1区 医学 Q1 CARDIAC & CARDIOVASCULAR SYSTEMS
Circulation: Heart Failure Pub Date : 2024-09-01 Epub Date: 2024-08-29 DOI:10.1161/CIRCHEARTFAILURE.124.011792
Christopher R deFilippi, Palak Shah, Sanjiv J Shah, Wendimagegn Alemayehu, Carolyn S P Lam, Javed Butler, Lothar Roessig, Christopher M O'Connor, Cynthia M Westerhout, Paul W Armstrong
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引用次数: 0

Abstract

Background: Heart failure with preserved ejection fraction (HFpEF) is a heterogeneous syndrome that may emerge from overlapping systemic processes associated with comorbidities. We assessed whether unique clusters of circulating proteins are associated with specific clinical characteristics and functional status at baseline and follow-up in a well-phenotyped cohort of patients with HFpEF.

Methods: We evaluated 368 proteins associated with cardiovascular disease and inflammation in prerandomization blood samples from 763 VITALITY-HFpEF (Vericiguat to Improve Physical Functioning in Daily Living Activities of Patients With HFpEF) participants who had a left ventricular ejection fraction ≥45% and a heart failure decompensation event within 6 months. Proteins were clustered, and their associations with clinical characteristics, baseline, and 24-week functional outcomes (Kansas City Cardiomyopathy Questionnaire Physical Limitation Score, 6-minute walk distance [6MWD], and Fried frailty phenotype) were estimated with linear regression. Elastic net regression was used to derive a proteomic summary composite to predict changes in 24-week functional outcomes.

Results: Four unique protein clusters were identified, containing 24, 66, 197, and 81 proteins. At baseline, 2 protein clusters with the hub proteins caspase-3 and Dickkopf-related protein 1 were associated with increased frailty, whereas the cluster with tumor necrosis factor receptor 1 as a hub protein was associated with lower Kansas City Cardiomyopathy Questionnaire Physical Limitation Score and shorter 6MWD. By contrast, the cluster with protein C as a hub protein was associated with less frailty and longer a 6MWD. The 24-week increase in 6MWD was negatively correlated with the protein cluster with caspase-3; the protein C cluster was correlated with less frailty at 24 weeks. The baseline proteomic summary composite predicted observed changes in Kansas City Cardiomyopathy Questionnaire Physical Limitation Score and 6MWD at 24 weeks (r=0.42 and 0.30; P<0.001 for both).

Conclusions: Proteomics differentiate specific baseline functional traits associated with HFpEF and may facilitate phenotyping in a heterogeneous disease. These proteins also provide insights into the diverse pathophysiology of HFpEF and which patients may improve functional status during follow-up.

Registration: URL: https://www.clinicaltrials.gov; Unique identifier: NCT03547583.

蛋白质组学识别射血分数保留型心力衰竭的临床表型并预测功能性结局:VITALITY-HFpEF 的启示。
背景:射血分数保留型心力衰竭(HFpEF)是一种异质性综合征,可能源于与合并症相关的重叠系统过程。我们在一个表型清晰的 HFpEF 患者队列中评估了独特的循环蛋白质群是否与基线和随访时的特定临床特征和功能状态相关:我们对763名左室射血分数≥45%且6个月内发生过心力衰竭失代偿事件的VITALITY-HFpEF(维力青改善HFpEF患者日常生活活动中的身体功能)参与者随机化前血液样本中与心血管疾病和炎症相关的368种蛋白质进行了评估。对蛋白质进行聚类,并通过线性回归估算其与临床特征、基线和 24 周功能结果(堪萨斯城心肌病问卷调查体力限制评分、6 分钟步行距离 [6MWD] 和弗里德虚弱表型)的相关性。采用弹性净回归法得出蛋白质组综合摘要,以预测 24 周功能结果的变化:结果:发现了四个独特的蛋白质群,分别包含 24、66、197 和 81 个蛋白质。基线时,以caspase-3和Dickkopf相关蛋白1为中心蛋白的2个蛋白质群与虚弱程度增加有关,而以肿瘤坏死因子受体1为中心蛋白的蛋白质群与堪萨斯城心肌病问卷调查体力限制评分降低和6MWD缩短有关。相比之下,以蛋白 C 为中心蛋白的群组与较轻的虚弱程度和较长的 6MWD 相关。24周后6MWD的增加与带有caspase-3的蛋白质群呈负相关;蛋白质C群与24周时虚弱程度较低有关。基线蛋白质组汇总综合结果预测了观察到的堪萨斯城心肌病问卷调查体力限制评分和24周时6MWD的变化(r=0.42和0.30;PC结论:蛋白质组学可区分与高频低氧血症相关的特定基线功能特征,有助于对异质性疾病进行表型分析。这些蛋白质还有助于深入了解 HFpEF 的不同病理生理学,以及哪些患者可能在随访期间改善功能状态:URL: https://www.clinicaltrials.gov; 唯一标识符:NCT03547583。
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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来源期刊
Circulation: Heart Failure
Circulation: Heart Failure 医学-心血管系统
CiteScore
12.90
自引率
3.10%
发文量
271
审稿时长
6-12 weeks
期刊介绍: Circulation: Heart Failure focuses on content related to heart failure, mechanical circulatory support, and heart transplant science and medicine. It considers studies conducted in humans or analyses of human data, as well as preclinical studies with direct clinical correlation or relevance. While primarily a clinical journal, it may publish novel basic and preclinical studies that significantly advance the field of heart failure.
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