Affiliation:
1. Department of Cardiology University Medical Center Groningen Groningen The Netherlands
2. Division of Experimental Cardiology, Department of Cardiology, Thorax Center Erasmus University Medical Center PO Box 2040 3000CA Rotterdam The Netherlands
3. Section of Cardio‐Oncology and Immunology, Division of Cardiology and the Cardiovascular Research Institute University of California San Francisco San Francisco CA USA
4. Department of Pharmacology, Assistance Publique‐Hôpitaux de Paris (AP‐HP) Sorbonne Université, INSERM, CIC‐1901, UNICO‐GRECO Cardio‐oncology Program Paris France
Abstract
AbstractAimsThere are limited data examining the role of immune checkpoint (IC) ligands in the pathophysiology of heart failure (HF). Therefore, we explore this in three HF animal models and in three different human cohorts (healthy, stable, and worsening HF).Methods and resultsTranscriptomic analyses of cardiac tissue of three different HF mouse models revealed differentially expressed IC receptors and their ligands compared with control mice. Based on this observation, serum levels of three well‐known IC ligands (i.e. sPD‐L1, sPD‐L2 and galectin‐9) were measured in stable HF patients from the Vitamin D Chronic Heart Failure (VitD‐CHF) study (n = 101), as well as healthy individuals from the Prevention of Renal and Vascular End‐stage Disease (PREVEND) study (n = 58). sPD‐L1, sPD‐L2, and galectin‐9 were all associated with New York Heart Association classification. In multivariate linear regression analyses, all three IC ligands were associated with galectin‐3 (β = 0.230, β = 0.283, and β = 0.304, respectively). sPD‐L1 and galectin‐9 were also associated with hs‐troponin‐T (β = 0.386 and β = 0.314). Regarding prognosis, higher serum levels of sPD‐L1 and galectin‐9 were significantly associated with increased risk for HF hospitalization and all‐cause mortality [hazard ratio 1.69 (1.09–2.59) and hazard ratio 1.50 (1.06–2.12)]. Furthermore, the importance of IC ligands was tested in another stage of HF, namely worsening HF patients. In the worsening HF cohort (The BIOlogy Study to Tailored Treatment in Chronic Heart Failure) (n = 2032), sPD‐L2 and galectin‐9 were associated with New York Heart Association classification and significantly predicted outcome with an increased relative risk of 15% and 20%, after multivariable adjustment, respectively.ConclusionsIC ligands are expressed in cardiac disease models, and serum levels of IC ligands are elevated in HF patients, are associated with disease severity, and significantly predict prognosis. These data indicate a potential role for IC ligands in HF pathogenesis.
Funder
Hartstichting
Fondation Leducq
European Research Council
Stichting De Cock-Hadders
Universitair Medisch Centrum Groningen
European Commission
Subject
Cardiology and Cardiovascular Medicine
Cited by
5 articles.
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