Cardiovascular‐kidney‐metabolic overlap in heart failure with preserved ejection fraction: Cardiac structure and function, clinical outcomes, and response to sacubitril/valsartan in PARAGON‐HF

医学 沙库比林、缬沙坦 沙库比林 射血分数 心力衰竭 缬沙坦 心脏病学 内科学 心功能曲线 肾功能 血压
作者
Mats Christian Højbjerg Lassen,John W. Ostrominski,Brian Claggett,Milton Packer,Michael R. Zile,Akshay S. Desai,Amil M. Shah,Maja Čikeš,Béla Merkely,Mauro Gori,Xiaowen Wang,Sheila M. Hegde,Marc A. Pfeffer,Martin Lefkowitz,John J.V. McMurray,Scott D. Solomon,Muthiah Vaduganathan
出处
期刊:European Journal of Heart Failure [Elsevier BV]
卷期号:26 (8): 1762-1774 被引量:10
标识
DOI:10.1002/ejhf.3304
摘要

Abstract Aims Cardiovascular‐kidney‐metabolic (CKM) multimorbidity is prevalent among individuals with heart failure (HF), but whether cardiac structure and function, clinical outcomes, and treatment response to sacubitril/valsartan vary in relation to CKM status is unknown. Methods and results In this PARAGON‐HF post‐hoc analysis, we evaluated the impact of CKM multimorbidity (atherosclerotic cardiovascular [CV] disease, chronic kidney disease, and type 2 diabetes) on cardiac structure and function, clinical outcomes, and treatment effects of sacubitril/valsartan versus valsartan. The primary outcome was a composite of total HF hospitalizations and CV death. Secondary outcomes included the individual components of the primary outcome and a composite kidney outcome (sustained estimated glomerular filtration rate reduction of ≥50%, end‐stage kidney disease, or kidney‐related death). At baseline, 35.2% had one CKM condition, 33.3% had two, 15.9% had three, and only 15.6% had HF alone. CKM multimorbidity was associated with higher septal and posterior wall thickness, lower global longitudinal strain, higher E/e', and worse right ventricular function. Total HF hospitalizations or CV death increased with greater CKM multimorbidity, with the highest relative risk observed with three CKM conditions (rate ratio 3.06, 95% confidence interval 2.33–4.03), compared with HF alone. Treatment effects of sacubitril/valsartan were consistent irrespective of the number of CKM conditions for the primary endpoint ( p interaction = 0.75), CV death ( p interaction = 0.82), total HF hospitalizations ( p interaction = 0.67), and the composite kidney endpoint ( p interaction = 0.99). Conclusions Cardiovascular‐kidney‐metabolic multimorbidity was common in PARAGON‐HF and associated with adverse changes in cardiac structure and function and with a stepwise increase in risk of clinical outcomes. Treatment effects of sacubitril/valsartan were consistent irrespective of CKM burden. Clinical Trial Registration: ClinicalTrials.gov NCT01920711.
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