Coordinated expression of BMP10/ALK1/endoglin—proteins that drive embryonic cardiac and vascular morphogenesis—in patients with heart failure: The EMPEROR Program

IF 10.8 1区医学 Q1 CARDIAC & CARDIOVASCULAR SYSTEMS

European Journal of Heart Failure Pub Date : 2025-07-15 DOI:10.1002/ejhf.3764

Milton Packer, Javed Butler, João Pedro Ferreira, Tariq Jamal Siddiqi, James L. Januzzi, Naveed Sattar, Sandra González Maldonado, Marina Panova‐Noeva, Jürgen H. Prochaska, Mikhail Sumin, Serge Masson, Stuart J. Pocock, Gerasimos Filippatos, Stefan D. Anker, Faiez Zannad

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引用次数: 0

Abstract

AimsBone morphogenetic protein 10 (BMP10), activin receptor‐like kinase 1 (ALK1) and endoglin form a single transforming growth factor‐β family signalling complex that is the principal driver of cardiac and vascular morphogenesis and maturation during hypoxic embryonic development. These proteins are down‐regulated with the onset of normoxia at birth, but are up‐regulated following experimental cardiac injury. Yet, little is known about the expression of this protein complex in patients with heart failure.Methods and resultsIn the EMPEROR Program, we measured serum levels of BMP10 by electrochemiluminescence immunoassay in 1127 patients in Cohort 1 (n = 1127) and plasma levels of BMP10, ALK1 and endoglin by proximity extension assay in a distinct Cohort 2 (n = 1120). In both cohorts, patients were characterized at baseline and were followed for the occurrence of major adverse heart failure events. Levels of BMP10, ALK1 and endoglin at baseline and changes in these levels during follow‐up were closely correlated with each other. Higher levels of BMP10, ALK1 and endoglin were associated with worse functional class, higher likelihood of atrial fibrillation and higher levels of natriuretic peptides and troponin T (p for trend <0.001 for all). Increasing levels of BMP10, ALK1 and endoglin were associated with progressively higher risks of major adverse outcomes (p for trend <0.001 for all three proteins and for all heart failure endpoints). The hazard ratios for the risks associated with tertiles of the three proteins in Cohort 2 were remarkably similar to those seen with BMP10 in Cohort 1. Treatment with empagliflozin had a modest effect to reduce BMP10 in both cohorts.ConclusionsThe coordinated circulating expression of proteins critical to foetal cardiac and vascular development tracks closely with the severity of heart failure, as reflected by symptoms, cardiac injury and stress, prevalence of atrial fibrillation and other comorbidities, and prognosis, suggesting a role of BMP10/ALK1/endoglin signalling in the progression of heart failure.

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在心力衰竭患者中驱动胚胎心脏和血管形态发生的BMP10/ALK1/内啡肽蛋白的协调表达：EMPEROR项目

目的：骨形态发生蛋白10 （BMP10）、激活素受体样激酶1 （ALK1）和内啡肽形成单一的转化生长因子β家族信号复合物，是缺氧胚胎发育过程中心脏和血管形态发生和成熟的主要驱动因素。这些蛋白在出生时正常缺氧时下调，但在实验性心脏损伤后上调。然而，人们对这种蛋白复合物在心力衰竭患者中的表达知之甚少。方法和结果在EMPEROR项目中，我们通过电化学发光免疫分析法测定了1127例队列1患者的血清BMP10水平（n = 1127），并通过邻近延伸法测定了不同队列2患者的血浆BMP10、ALK1和内啡肽水平（n = 1120）。在这两个队列中，患者在基线时进行特征描述，并随访主要不良心力衰竭事件的发生情况。基线时BMP10、ALK1和内啡肽水平与随访期间这些水平的变化密切相关。较高水平的BMP10、ALK1和内啡肽与较差的功能等级、较高的房颤可能性和较高水平的利钠肽和肌钙蛋白T相关（趋势p = 0.001）。BMP10、ALK1和内啡肽水平的升高与主要不良结局的风险逐渐升高相关（所有三种蛋白和所有心力衰竭终点的趋势p为0.001）。队列2中与三种蛋白质含量相关的风险风险比与队列1中与BMP10相关的风险风险比非常相似。在两个队列中，恩格列净治疗对降低BMP10有中等效果。结论对胎儿心脏和血管发育至关重要的蛋白的循环表达与心衰的严重程度密切相关，如症状、心脏损伤和应激、房颤和其他合并症的患病率以及预后，提示BMP10/ALK1/内啡肽信号在心衰的进展中发挥作用。

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来源期刊

European Journal of Heart Failure 医学-心血管系统

CiteScore

27.30

自引率

11.50%

发文量

365

审稿时长

1 months

期刊介绍： European Journal of Heart Failure is an international journal dedicated to advancing knowledge in the field of heart failure management. The journal publishes reviews and editorials aimed at improving understanding, prevention, investigation, and treatment of heart failure. It covers various disciplines such as molecular and cellular biology, pathology, physiology, electrophysiology, pharmacology, clinical sciences, social sciences, and population sciences. The journal welcomes submissions of manuscripts on basic, clinical, and population sciences, as well as original contributions on nursing, care of the elderly, primary care, health economics, and other related specialist fields. It is published monthly and has a readership that includes cardiologists, emergency room physicians, intensivists, internists, general physicians, cardiac nurses, diabetologists, epidemiologists, basic scientists focusing on cardiovascular research, and those working in rehabilitation. The journal is abstracted and indexed in various databases such as Academic Search, Embase, MEDLINE/PubMed, and Science Citation Index.