Targeting Cyclophilin A in the Cardiac Microenvironment Preserves Heart Function and Structure in Failing Hearts.

Sigle, Manuel; Rohlfing, Anne-Katrin; Cruz Santos, Melanie; Kopp, Timo; Krutzke, Konstantin; Gidlund, Vincent; Kollotzek, Ferdinand; Marzi, Julia; von Ungern-Sternberg, Saskia; Poso, Antti; Heikenwälder, Mathias; Schenke-Layland, Katja; Seizer, Peter; Möllmann, Julia; Marx, Nikolaus; Feil, Robert; Feil, Susanne; Lukowski, Robert; Borst, Oliver; Schäffer, Tilman E; Müller, Karin Anne Lydia; Gawaz, Meinrad P; Heinzmann, David

Sigle, Manuel; Rohlfing, Anne-Katrin; Cruz Santos, Melanie; Kopp, Timo; Krutzke, Konstantin; Gidlund, Vincent; Kollotzek, Ferdinand; Marzi, Julia; von Ungern-Sternberg, Saskia; Poso, Antti; Heikenwälder, Mathias; Schenke-Layland, Katja; Seizer, Peter; Möllmann, Julia; Marx, Nikolaus; Feil, Robert; Feil, Susanne; Lukowski, Robert; Borst, Oliver; Schäffer, Tilman E; Müller, Karin Anne Lydia; Gawaz, Meinrad P; Heinzmann, David.

Afiliación

Sigle M; Department of Cardiology and Angiology, Eberhard Karls University Tübingen, Germany. (M.S., A.-K.R., F.K., S.U.-S., P.S., O.B., K.A.L.M., M.P.G., D.H.).
Rohlfing AK; Department of Cardiology and Angiology, Eberhard Karls University Tübingen, Germany. (M.S., A.-K.R., F.K., S.U.-S., P.S., O.B., K.A.L.M., M.P.G., D.H.).
Cruz Santos M; Institute of Pharmacy, Pharmacology, Toxicology and Clinical Pharmacy, University of Tübingen, Germany. (M.C.S., R.L.).
Kopp T; Interfaculty Institute of Biochemistry (IFIB), University of Tübingen, Germany. (T.K., R.F., S.F.).
Krutzke K; Institute for Applied Physics, University of Tübingen, Germany. (K.K., V.G., T.E.S.).
Gidlund V; Institute for Applied Physics, University of Tübingen, Germany. (K.K., V.G., T.E.S.).
Kollotzek F; Department of Cardiology and Angiology, Eberhard Karls University Tübingen, Germany. (M.S., A.-K.R., F.K., S.U.-S., P.S., O.B., K.A.L.M., M.P.G., D.H.).
Marzi J; DFG Heisenberg Group Cardiovascular Thrombo-Inflammation and Translational Thrombocardiology, University of Tübingen, Germany. (F.K., O.B.).
von Ungern-Sternberg S; Institute of Biomedical Engineering, Department for Medical Technologies and Regenerative Medicine, Eberhard Karls University Tübingen, Germany. (J. Marzi, K.S.-L.).
Poso A; Cluster of Excellence iFIT (EXC 2180) "Image-Guided and Functionally Instructed Tumor Therapies,", University of Tübingen, Germany. (J. Marzi, A.P., K.S.-L.).
Heikenwälder M; NMI Natural and Medical Sciences Institute at the University of Tübingen Reutlingen, Germany (J. Marzi, K.S.-L.).
Schenke-Layland K; Department of Cardiology and Angiology, Eberhard Karls University Tübingen, Germany. (M.S., A.-K.R., F.K., S.U.-S., P.S., O.B., K.A.L.M., M.P.G., D.H.).
Seizer P; Now with Center for Thrombosis and Hemostasis (CTH), University Medical Center of the Johannes Gutenberg-University Mainz, Germany (S.U.-S.).
Möllmann J; Cluster of Excellence iFIT (EXC 2180) "Image-Guided and Functionally Instructed Tumor Therapies,", University of Tübingen, Germany. (J. Marzi, A.P., K.S.-L.).
Marx N; School of Pharmacy, Faculty of Health Sciences, University of Eastern Finland Kuopio (A.P.).
Feil R; Department of Pharmaceutical and Medicinal Chemistry, Institute of Pharmaceutical Sciences, Eberhard-Karls-Universität Tübingen, Germany (A.P.).
Feil S; Tübingen Center for Academic Drug Discovery and Development (TüCAD2), Tübingen, Germany (A.P.).
Lukowski R; Division of Chronic Inflammation and Cancer, German Cancer Research Centre Heidelberg (DKFZ), Germany (M.H.).
Borst O; University Tübingen, Faculty of Medicine, Institute for Interdisciplinary Research on Cancer Metabolism and Chronic Inflammation, M3-Research Center for Malignome, Metabolome and Microbiome (M.H.).
Schäffer TE; Institute of Biomedical Engineering, Department for Medical Technologies and Regenerative Medicine, Eberhard Karls University Tübingen, Germany. (J. Marzi, K.S.-L.).
Müller KAL; Cluster of Excellence iFIT (EXC 2180) "Image-Guided and Functionally Instructed Tumor Therapies,", University of Tübingen, Germany. (J. Marzi, A.P., K.S.-L.).
Gawaz MP; NMI Natural and Medical Sciences Institute at the University of Tübingen Reutlingen, Germany (J. Marzi, K.S.-L.).
Heinzmann D; Department of Cardiology and Angiology, Eberhard Karls University Tübingen, Germany. (M.S., A.-K.R., F.K., S.U.-S., P.S., O.B., K.A.L.M., M.P.G., D.H.).

Circ Res ; 2024 Aug 14.

Article en En | MEDLINE | ID: mdl-39140165

ABSTRACT

ABSTRACT

BACKGROUND:

Cardiac hypertrophy is characterized by remodeling of the myocardium, which involves alterations in the ECM (extracellular matrix) and cardiomyocyte structure. These alterations critically contribute to impaired contractility and relaxation, ultimately leading to heart failure. Emerging evidence implicates that extracellular signaling molecules are critically involved in the pathogenesis of cardiac hypertrophy and remodeling. The immunophilin CyPA (cyclophilin A) has been identified as a potential culprit. In this study, we aimed to unravel the interplay between eCyPA (extracellular CyPA) and myocardial dysfunction and evaluate the therapeutic potential of inhibiting its extracellular accumulation to improve heart function.

METHODS:

Employing a multidisciplinary approach encompassing in silico, in vitro, in vivo, and ex vivo experiments we studied a mouse model of cardiac hypertrophy and human heart specimen to decipher the interaction of CyPA and the cardiac microenvironment in highly relevant pre-/clinical settings. Myocardial expression of CyPA (immunohistology) and the inflammatory transcriptome (NanoString) was analyzed in human cardiac tissue derived from patients with nonischemic, noninflammatory congestive heart failure (n=187). These analyses were paralleled by a mouse model of Ang (angiotensin) II-induced heart failure, which was assessed by functional (echocardiography), structural (immunohistology, atomic force microscopy), and biomolecular (Raman spectroscopy) analyses. The effect of inhibiting eCyPA in the cardiac microenvironment was evaluated using a newly developed neutralizing anti-eCyPA monoclonal antibody.

RESULTS:

We observed a significant accumulation of eCyPA in both human and murine-failing hearts. Importantly, higher eCyPA expression was associated with poor clinical outcomes in patients (P=0.043) and contractile dysfunction in mice (Pearson correlation coefficient, -0.73). Further, myocardial expression of eCyPA was critically associated with an increase in myocardial hypertrophy, inflammation, fibrosis, stiffness, and cardiac dysfunction in vivo. Antibody-based inhibition of eCyPA prevented (Ang II)-induced myocardial remodeling and dysfunction in mice.

CONCLUSIONS:

Our study provides strong evidence of the pathogenic role of eCyPA in remodeling, myocardial stiffening, and dysfunction in heart failure. The findings suggest that antibody-based inhibition of eCyPA may offer a novel therapeutic strategy for nonischemic heart failure. Further research is needed to evaluate the translational potential of these interventions in human patients with cardiac hypertrophy.

Palabras clave

contractility; cyclophilin A; hypertrophy; inflammation; myocardium

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Texto completo: 1 Colección: 01-internacional Banco de datos: MEDLINE Idioma: En Revista: Circ Res Año: 2024 Tipo del documento: Article

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Texto completo: 1 Colección: 01-internacional Banco de datos: MEDLINE Idioma: En Revista: Circ Res Año: 2024 Tipo del documento: Article