Shedding of syndecan-4 promotes immune cell recruitment and mitigates cardiac dysfunction after lipopolysaccharide challenge in mice

Mari E Strand; Jan Magnus Aronsen; Bjørn Braathen; Ivar Sjaastad; Heidi Kvaløy; Theis Tønnessen; Geir Christensen; Ida G Lunde

doi:10.1016/j.yjmcc.2015.10.003

Shedding of syndecan-4 promotes immune cell recruitment and mitigates cardiac dysfunction after lipopolysaccharide challenge in mice

J Mol Cell Cardiol. 2015 Nov:88:133-44. doi: 10.1016/j.yjmcc.2015.10.003. Epub 2015 Oct 9.

Authors

Mari E Strand¹, Jan Magnus Aronsen², Bjørn Braathen³, Ivar Sjaastad⁴, Heidi Kvaløy⁴, Theis Tønnessen⁵, Geir Christensen⁴, Ida G Lunde⁶

Affiliations

¹ Institute for Experimental Medical Research, Oslo University Hospital and University of Oslo, Oslo, Norway; KG Jebsen Cardiac Research Center and Center for Heart Failure Research, University of Oslo, Oslo, Norway. Electronic address: m.e.strand@medisin.uio.no.
² Bjørknes College, Oslo, Norway.
³ Department of Cardiothoracic Surgery, Oslo University Hospital Ullevål, Oslo, Norway.
⁴ Institute for Experimental Medical Research, Oslo University Hospital and University of Oslo, Oslo, Norway; KG Jebsen Cardiac Research Center and Center for Heart Failure Research, University of Oslo, Oslo, Norway.
⁵ KG Jebsen Cardiac Research Center and Center for Heart Failure Research, University of Oslo, Oslo, Norway; Department of Cardiothoracic Surgery, Oslo University Hospital Ullevål, Oslo, Norway.
⁶ Institute for Experimental Medical Research, Oslo University Hospital and University of Oslo, Oslo, Norway; KG Jebsen Cardiac Research Center and Center for Heart Failure Research, University of Oslo, Oslo, Norway; Department of Genetics, Harvard Medical School, Boston MA, USA.

PMID: 26449522
DOI: 10.1016/j.yjmcc.2015.10.003

Abstract

Inflammation is central to heart failure progression. Innate immune signaling increases expression of the transmembrane proteoglycan syndecan-4 in cardiac myocytes and fibroblasts, followed by shedding of its ectodomain. Circulating shed syndecan-4 is increased in heart failure patients, however the pathophysiological and molecular consequences associated with syndecan-4 shedding remain poorly understood. Here we used lipopolysaccharide (LPS) challenge to investigate the effects of syndecan-4 shedding in the heart. Wild-type mice (10mg/kg, 9h) and cultured neonatal rat cardiomyocytes and fibroblasts were subjected to LPS challenge. LPS increased cardiac syndecan-4 mRNA without altering full-length protein. Elevated levels of shedding fragments in the myocardium and blood from the heart confirmed syndecan-4 shedding in vivo. A parallel upregulation of ADAMTS1, ADAMTS4 and MMP9 mRNA suggested these shedding enzymes to be involved. Echocardiography revealed reduced ejection fraction, diastolic tissue velocity and prolonged QRS duration in mice unable to shed syndecan-4 (syndecan-4 KO) after LPS challenge. In line with syndecan-4 shedding promoting immune cell recruitment, expression of immune cell markers (CD8, CD11a, F4/80) and adhesion receptors (Icam1, Vcam1) were attenuated in syndecan-4 KO hearts after LPS. Cardiomyocytes and fibroblasts exposed to shed heparan sulfate-substituted syndecan-4 ectodomains showed increased Icam1, Vcam1, TNFα and IL-1β expression and NF-κB-activation, suggesting direct regulation of immune cell recruitment pathways. In cardiac fibroblasts, shed ectodomains regulated expression of extracellular matrix constituents associated with collagen synthesis, cross-linking and turnover. Higher syndecan-4 levels in the coronary sinus vs. the radial artery of open heart surgery patients suggested that syndecan-4 is shed from the human heart. Our data demonstrate that shedding of syndecan-4 ectodomains is part of the cardiac innate immune response, promoting immune cell recruitment, extracellular matrix remodeling and mitigating cardiac dysfunction in response to LPS.

Keywords: Fibrosis; Heart failure; Innate immunity; Proteoglycan; Sepsis.

Publication types

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

MeSH terms

ADAM Proteins / genetics
ADAM Proteins / immunology
ADAMTS1 Protein
ADAMTS4 Protein
Animals
Antigens, CD / genetics
Antigens, CD / immunology
Antigens, Differentiation / genetics
Antigens, Differentiation / immunology
Fibroblasts / drug effects
Fibroblasts / immunology
Fibroblasts / pathology
Gene Expression Regulation
HEK293 Cells
Heart Failure / chemically induced
Heart Failure / immunology*
Heart Failure / pathology
Heart Failure / prevention & control
Humans
Injections, Intraperitoneal
Intercellular Adhesion Molecule-1 / genetics
Intercellular Adhesion Molecule-1 / immunology
Lipopolysaccharides
Male
Matrix Metalloproteinase 9 / genetics
Matrix Metalloproteinase 9 / immunology
Mice
Mice, Inbred C57BL
Myocytes, Cardiac / drug effects
Myocytes, Cardiac / immunology*
Myocytes, Cardiac / pathology
Neutrophil Infiltration / drug effects
Procollagen N-Endopeptidase / genetics
Procollagen N-Endopeptidase / immunology
Rats
Rats, Wistar
Sepsis / chemically induced
Sepsis / immunology*
Sepsis / pathology
Sepsis / prevention & control
Signal Transduction
Stroke Volume
Syndecan-4 / genetics
Syndecan-4 / immunology*
Syndecan-4 / metabolism
Vascular Cell Adhesion Molecule-1 / genetics
Vascular Cell Adhesion Molecule-1 / immunology

Substances

Antigens, CD
Antigens, Differentiation
Lipopolysaccharides
Sdc4 protein, mouse
Syndecan-4
Vascular Cell Adhesion Molecule-1
monocyte-macrophage differentiation antigen
Intercellular Adhesion Molecule-1
ADAM Proteins
ADAMTS1 Protein
Adamts1 protein, mouse
Procollagen N-Endopeptidase
Matrix Metalloproteinase 9
Mmp9 protein, mouse
ADAMTS4 Protein
ADAMTS4 protein, human
Adamts4 protein, mouse