Inhibition of the extracellular enzyme A disintegrin and metalloprotease with thrombospondin motif 4 prevents cardiac fibrosis and dysfunction

Maria Vistnes; Pugazendhi Murugan Erusappan; Athiramol Sasi; Einar Sjaastad Nordén; Kaja Knudsen Bergo; Andreas Romaine; Ida Gjervold Lunde; Lili Zhang; Maria Belland Olsen; Jonas Øgaard; Cathrine Rein Carlson; Christian Hjorth Wang; Jon Riise; Christen Peder Dahl; Arnt Eltvedt Fiane; Ida Marie Hauge-Iversen; Emil Espe; Arne Olav Melleby; Theis Tønnessen; Jan Magnus Aronsen; Ivar Sjaastad; Geir Christensen

doi:10.1093/cvr/cvad078

Inhibition of the extracellular enzyme A disintegrin and metalloprotease with thrombospondin motif 4 prevents cardiac fibrosis and dysfunction

Cardiovasc Res. 2023 Aug 19;119(10):1915-1927. doi: 10.1093/cvr/cvad078.

Authors

Maria Vistnes^{1

2

3

4}, Pugazendhi Murugan Erusappan^{1

2}, Athiramol Sasi^{1

2}, Einar Sjaastad Nordén^{1

2}, Kaja Knudsen Bergo^{1

2}, Andreas Romaine^{1

2}, Ida Gjervold Lunde^{1

2}, Lili Zhang^{1

2}, Maria Belland Olsen⁵, Jonas Øgaard⁵, Cathrine Rein Carlson¹, Christian Hjorth Wang⁴, Jon Riise⁶, Christen Peder Dahl⁷, Arnt Eltvedt Fiane^{8

9}, Ida Marie Hauge-Iversen^{1

2}, Emil Espe^{1

2}, Arne Olav Melleby^{1

10}, Theis Tønnessen^{1

2

8}, Jan Magnus Aronsen^{9

10

11}, Ivar Sjaastad^{1

2}, Geir Christensen^{1

2}

Affiliations

¹ Institute for Experimental Medical Research, Oslo University Hospital and University of Oslo, Kirkeveien 166, 0450 Oslo, Norway.
² K.G. Jebsen Center for Cardiac Research, University of Oslo, Kirkeveien 166, 0450 Oslo, Norway.
³ Department of Cardiology, Oslo University Hospital Ullevål, Kirkeveien 166, 0450 Oslo, Norway.
⁴ Department of Internal Medicine, Diakonhjemmet Hospital, Diakonveien 12, 0370 Oslo, Norway.
⁵ Research Institute of Internal Medicine, Oslo University Hospital and University of Oslo, Sognsvannsveien 20, 0372 Oslo, Norway.
⁶ Department of Oncology, Oslo University Hospital, Ullernchausseen 70, 0379 Oslo, Norway.
⁷ Department of Cardiology, Oslo University Hospital Rikshospitalet, Sognsvannsveien 20, 0372 Oslo, Norway.
⁸ Department of Cardiothoracic Surgery, Oslo University Hospital, Sognsvannsveien 20, 0372 Oslo, Norway.
⁹ Faculty of Medicine, University of Oslo, Klaus Torgårdsvei 3, 0372 Oslo, Norway.
¹⁰ Department of Molecular Medicine, Institute of Basic Medical Sciences, University of Oslo, Sognsvannsveien 9, 0372 Oslo, Norway.
¹¹ Department of Pharmacology, Oslo University Hospital Rikshospitalet, Sognsvannsveien 20, 0372 Oslo, Norway.

Abstract

Aims: Heart failure is a condition with high mortality rates, and there is a lack of therapies that directly target maladaptive changes in the extracellular matrix (ECM), such as fibrosis. We investigated whether the ECM enzyme known as A disintegrin and metalloprotease with thrombospondin motif (ADAMTS) 4 might serve as a therapeutic target in treatment of heart failure and cardiac fibrosis.

Methods and results: The effects of pharmacological ADAMTS4 inhibition on cardiac function and fibrosis were examined in rats exposed to cardiac pressure overload. Disease mechanisms affected by the treatment were identified based on changes in the myocardial transcriptome. Following aortic banding, rats receiving an ADAMTS inhibitor, with high inhibitory capacity for ADAMTS4, showed substantially better cardiac function than vehicle-treated rats, including ∼30% reduction in E/e' and left atrial diameter, indicating an improvement in diastolic function. ADAMTS inhibition also resulted in a marked reduction in myocardial collagen content and a down-regulation of transforming growth factor (TGF)-β target genes. The mechanism for the beneficial effects of ADAMTS inhibition was further studied in cultured human cardiac fibroblasts producing mature ECM. ADAMTS4 caused a 50% increase in the TGF-β levels in the medium. Simultaneously, ADAMTS4 elicited a not previously known cleavage of TGF-β-binding proteins, i.e. latent-binding protein of TGF-β and extra domain A-fibronectin. These effects were abolished by the ADAMTS inhibitor. In failing human hearts, we observed a marked increase in ADAMTS4 expression and cleavage activity.

Conclusion: Inhibition of ADAMTS4 improves cardiac function and reduces collagen accumulation in rats with cardiac pressure overload, possibly through a not previously known cleavage of molecules that control TGF-β availability. Targeting ADAMTS4 may serve as a novel strategy in heart failure treatment, in particular, in heart failure with fibrosis and diastolic dysfunction.

Keywords: ADAMTS enzymes; Cardiac fibrosis; Extracellular matrix; Heart failure; New therapy.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Cardiomyopathies* / metabolism
Collagen / metabolism
Disintegrins / metabolism
Disintegrins / pharmacology
Fibroblasts / metabolism
Fibrosis
Heart Failure* / metabolism
Humans
Metalloproteases / metabolism
Metalloproteases / pharmacology
Myocardium / metabolism
Rats
Thrombospondins / metabolism
Transforming Growth Factor beta / metabolism

Substances

Disintegrins
Collagen
Transforming Growth Factor beta
Thrombospondins
Metalloproteases