The Role of the Thrombospondins in Healing Myocardial Infarcts

Chatila, Khaled; Ren, Guofeng; Xia, Ying; Huebener, Peter; Bujak, Marcin; Frangogiannis, Nikolaos G.

doi:10.2174/187152507779315813

Cited by 51 publications

(43 citation statements)

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“…Our findings suggested that the selective endogenous expression of TSP-1 in the infarct border zone may protect the non-infarcted myocardium from inflammatory cell infiltration and fibrotic remodeling. Several distinct TSP-1-mediated actions may be responsible for its protective effects [332]. First, enhanced TGF-β activation in the border zone may locally suppress inflammatory mediator synthesis.…”

Section: The Infarct Border Zone As a Barrier Preventing Expansion Ofmentioning

confidence: 99%

The immune system and cardiac repair

Frangogiannis

2008

Pharmacological Research

568

499

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Myocardial infarction is the most common cause of cardiac injury and results in acute loss of a large number of myocardial cells. Because the heart has negligible regenerative capacity, cardiomyocyte death triggers a reparative response that ultimately results in formation of a scar and is associated with dilative remodeling of the ventricle. Cardiac injury activates innate immune mechanisms initiating an inflammatory reaction. Toll Like Receptor-mediated pathways, the complement cascade and reactive oxygen generation induce Nuclear Factor (NF)-κB activation and upregulate chemokine and cytokine synthesis in the infarcted heart. Chemokines stimulate the chemotactic recruitment of inflammatory leukocytes into the infarct, while cytokines promote adhesive interactions between leukocytes and endothelial cells, resulting in transmigration of inflammatory cells into the site of injury. Monocyte subsets play distinct roles in phagocytosis of dead cardiomyocytes and in granulation tissue formation through the release of growth factors. Clearance of dead cells and matrix debris may be essential for resolution of inflammation and transition into the reparative phase. Transforming Growth Factor (TGF)-β plays a crucial role in cardiac repair by suppressing inflammation while promoting myofibroblast phenotypic modulation and extracellular matrix deposition. Myofibroblast proliferation and angiogenesis result in formation of highly vascularized granulation tissue. As the healing infarct matures, fibroblasts become apoptotic and a collagen-based matrix is formed, while many infarct neovessels acquire a muscular coat and uncoated vessels regress. Timely resolution of the inflammatory infiltrate and spatial containment of the inflammatory and reparative response into the infarcted area are essential for optimal infarct healing. Targeting inflammatory pathways following infarction may reduce cardiomyocyte injury and attenuate adverse remodeling. In addition, understanding the role of the immune system in cardiac repair is necessary in order to design optimal strategies for cardiac regeneration.

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Section: The Infarct Border Zone As a Barrier Preventing Expansion Ofmentioning

confidence: 99%

The immune system and cardiac repair

Frangogiannis

2008

Pharmacological Research

568

499

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“…Therefore, it is no surprise that CD44, which is involved in the ECM-receptor interaction, was found to be downregulated in the current study. Chatila et al (38) also found that certain compositions of the infarct border zone may slow down left ventricular remodeling by suppressing inflammation. In the current study, GO terms enriched by downregulated genes were mainly associated with the stimulus and immune response.…”

Section: Genementioning

confidence: 96%

Identification of nondiabetic heart failure-associated genes by bioinformatics approaches in patients with dilated ischemic cardiomyopathy

Zhang

Liu³

et al. 2016

Experimental and Therapeutic Medicine

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Heart failure (HF) is a common pathological condition affecting 4% of the worldwide population. However, approaches for predicting or treating nondiabetic HF (ND-HF) progression are insufficient. In the current study, the gene expression profile GSE26887 was analyzed, which contained samples from 5 healthy controls, 7 diabetes mellitus-HF patients and 12 ND-HF patients with dilated ischemic cardiomyopathy. The dataset of 5 healthy controls and 12 ND-HF patients was normalized with robust multichip average analysis and the differentially expressed genes (DEGs) were screened by unequal variance t-test and multiple-testing correction. In addition, the protein-protein interaction (PPI) network of the upregulated and downregulated genes was constructed using the Search Tool for the Retrieval of Interacting Genes/Proteins database and the Cytoscape software platform. Subsequently, gene ontology (GO) and Kyoto Encyclopedia of Genes and Genomes (KEGG) pathway enrichment analyses were performed. A total of 122 upregulated and 133 downregulated genes were detected. The most significantly up- and downregulated genes were and, respectively. In addition, 38 and 77 nodes were obtained in the up- and downregulated PPI network. DEGs that owned the highest connectivity degree were and in the upregulated network, and in the downregulated networks, respectively. and were also found to be hub genes in the PPI network. Several GO terms and pathways that were enriched by DEGs were identified, and the most significantly enriched KEGG pathways were drug metabolism and extracellular matrix-receptor interaction. In conclusion, the two DEGs, and , may be important in the pathogenesis of HF and may be used for the diagnosis and treatment of HF.

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“…For example, low-density lipoprotein receptor-related protein (LRP) is a versatile scavenger and signaling receptor that binds multiple unrelated ligands and influences a wide variety of biological processes (reviewed by Lillis et al [58]). Since TIMP1 and -2, either alone or complexed with proMMP-2 or -9, respectively, can interact with LRP, it will be of particular interest to investigate whether LRP represents (i) a 'mitogenic' receptor for TIMPs; as it is the 'motogenic' receptor for plasminogen activator inhibitor-1 [59], and/ [58,60,61]. LRP is able to bind thrombospondin-1 and -2, two matricellular proteins that seem to be crucial regulators of the cardiac integrity necessary for the myocardium to cope with increased loading or ischemic stress [60,61].…”

Section: Exploring Receptor-mediated Pathways and Processes In Cardiamentioning

confidence: 99%

“…Since TIMP1 and -2, either alone or complexed with proMMP-2 or -9, respectively, can interact with LRP, it will be of particular interest to investigate whether LRP represents (i) a 'mitogenic' receptor for TIMPs; as it is the 'motogenic' receptor for plasminogen activator inhibitor-1 [59], and/ [58,60,61]. LRP is able to bind thrombospondin-1 and -2, two matricellular proteins that seem to be crucial regulators of the cardiac integrity necessary for the myocardium to cope with increased loading or ischemic stress [60,61]. Interestingly, the proMMP-2/TIMP-2/thrombospondin-triplex can be scavenged via LRP-mediated endocytosis, regulating the levels of both MMP-2 and TIMP-2 in the extracellular cardiac matrix.…”

Section: Exploring Receptor-mediated Pathways and Processes In Cardiamentioning

confidence: 99%

TIMPs and cardiac remodeling: ‘Embracing the MMP-independent-side of the family’

Vanhoutte¹,

Heymans

2010

Journal of Molecular and Cellular Cardiology

124

103

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a b s t r a c t a r t i c l e i n f oUnraveling the biological role of tissue inhibitors of metalloproteinases (TIMPs) during cardiac remodeling and the progression of heart failure has proven to be an enormous challenge. Remodeling of the cardiac extracellular matrix (ECM), regulated by matrix metalloproteinases (MMPs) and their endogenous inhibitors, TIMPs, is a well-established paradigm in cardiac health and disease. Originally, TIMPs were thought to function exclusively as endogenous inhibitors of MMP activity, thereby fine-tuning MMPmediated ECM degradation and numerous related processes. However, during the last two decades, the concept of MMP-independent TIMP-mediated receptor signaling and regulation of cell fate has emerged. Although our current knowledge is still limited, in this review, we highlight some of the novel data, illustrating the MMP-independent biological properties of the four TIMP family members. Moreover, we discuss how these cell-specific insights may contribute to the process of cardiac remodeling, disease and failure. Finally, we identify where additional research is needed that will codetermine the possible future of TIMPs as therapeutic targets.

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The Role of the Thrombospondins in Healing Myocardial Infarcts

Cited by 51 publications

References 0 publications

The immune system and cardiac repair

The immune system and cardiac repair

Identification of nondiabetic heart failure-associated genes by bioinformatics approaches in patients with dilated ischemic cardiomyopathy

TIMPs and cardiac remodeling: ‘Embracing the MMP-independent-side of the family’

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