Cardiac Overexpression of Monocyte Chemoattractant Protein-1 in Transgenic Mice Prevents Cardiac Dysfunction and Remodeling After Myocardial Infarction

Morimoto, Hajime; Takahashi, Masafumi; Izawa, Atsushi; Ise, Hirohiko; Hongo, Minoru; Kolattukudy, Pappachan E.; Ikeda, Uichi

doi:10.1161/01.res.0000246113.82111.2d

Cited by 138 publications

(113 citation statements)

References 33 publications

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“…Recent studies demonstrated that disruption of C/ EBP signaling in the adult epicardium reduced injury-induced neutrophil infiltration and improved cardiac function (19). However, both positive (20)(21)(22) and negative (23)(24)(25)(26) correlations between tissue remodeling and monocytes, and their lineage descendant macrophages, have been reported. CCL2, a chemokine that recruits and activates monocytes, seems to play a dual role in MI.…”

Section: Introductionmentioning

confidence: 99%

“…CCL2, a chemokine that recruits and activates monocytes, seems to play a dual role in MI. Targeted deletion of the CCL2 receptor (CCR2) improved left ventricular dilation and dysfunction (20,21), while cardiac overexpression of CCL2 also improved outcome (23) by inducing macrophages infiltration, angiogenesis, myocardial IL-6 secretion, and accumulation of cardiac myofibroblasts. Biphasic recruitment of Ly-6C hi and Ly-6C lo monocyte subsets from the spleen also promotes infarct healing (26)(27)(28)(29).…”

Section: Introductionmentioning

confidence: 99%

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Macrophages are required for neonatal heart regeneration

Aurora¹,

et al. 2014

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Myocardial infarction (MI) leads to cardiomyocyte death, which triggers an immune response that clears debris and restores tissue integrity. In the adult heart, the immune system facilitates scar formation, which repairs the damaged myocardium but compromises cardiac function. In neonatal mice, the heart can regenerate fully without scarring following MI; however, this regenerative capacity is lost by P7. The signals that govern neonatal heart regeneration are unknown. By comparing the immune response to MI in mice at P1 and P14, we identified differences in the magnitude and kinetics of monocyte and macrophage responses to injury. Using a cell-depletion model, we determined that heart regeneration and neoangiogenesis following MI depends on neonatal macrophages. Neonates depleted of macrophages were unable to regenerate myocardia and formed fibrotic scars, resulting in reduced cardiac function and angiogenesis. Immunophenotyping and gene expression profiling of cardiac macrophages from regenerating and nonregenerating hearts indicated that regenerative macrophages have a unique polarization phenotype and secrete numerous soluble factors that may facilitate the formation of new myocardium. Our findings suggest that macrophages provide necessary signals to drive angiogenesis and regeneration of the neonatal mouse heart. Modulating inflammation may provide a key therapeutic strategy to support heart regeneration.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Macrophages are required for neonatal heart regeneration

Aurora¹,

et al. 2014

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“…There is evidence that inflammation contributes to end organ damage (20). We have shown that in ANG IIinduced hypertension (32), as well as in renovascular hypertension (25,35), mineralocorticoid-salt hypertension (26,28), spontaneously hypertensive rats (9), and heart failure postmyocardial infarction (24), N-acetyl-seryl-aspartyl-lysyl-proline (Ac-SDKP) not only prevents but also reverses inflammation, cell proliferation, and fibrosis in the heart and kidney.…”

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confidence: 99%

Novel anti-inflammatory mechanisms ofN-Acetyl-Ser-Asp-Lys-Pro in hypertension-induced target organ damage

Sharma

Rhaleb

Pokharel

et al. 2008

American Journal of Physiology-Heart and Circulatory Physiology

121

108

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High blood pressure (HBP) is an important risk factor for cardiac, renal, and vascular dysfunction. Excess inflammation is the major pathogenic mechanism for HBPinduced target organ damage (TOD). N-acetyl-Ser-Asp-Lys-Pro (Ac-SDKP), a tetrapeptide specifically degraded by angiotensin converting enzyme (ACE), reduces inflammation, fibrosis, and TOD induced by HBP. Our hypothesis is that Ac-SDKP exerts its anti-inflammatory effects by inhibiting: 1) differentiation of bone marrow stem cells (BMSC) to macrophages, 2) activation and migration of macrophages, and 3) release of the proinflammatory cytokine TNF-␣ by activated macrophages. BMSC were freshly isolated and cultured in macrophage growth medium. Differentiation of murine BMSC to macrophages was analyzed by flow cytometry using F4/80 as a marker of macrophage maturation. Macrophage migration was measured in a modified Boyden chamber. TNF-␣ release by activated macrophages in culture was measured by ELISA. Myocardial macrophage activation in mice with ANG II-induced hypertension was studied by Western blotting of Mac-2 (galectin-3) protein. Interstitial collagen deposition was measured by picrosirius red staining. We found that Ac-SDKP (10 nM) reduced differentiation of cultured BMSC to mature macrophages by 24.5% [F4/80 positivity: 14.09 Ϯ 1.06 mean fluorescent intensity for vehicle and 10.63 Ϯ 0.35 for Ac-SDKP; P Ͻ 0.05]. Ac-SDKP also decreased galectin-3 and macrophage colonystimulating factor-dependent macrophage migration. In addition, Ac-SDKP decreased secretion of TNF-␣ by macrophages stimulated with bacterial LPS. In mice with ANG II-induced hypertension, Ac-SDKP reduced expression of galectin-3, a protein produced by infiltrating macrophages in the myocardium, and interstitial collagen deposition. In conclusion, this study demonstrates that part of the anti-inflammatory effect of Ac-SDKP is due to its direct effect on BMSC and macrophage, inhibiting their differentiation, activation, and cytokine release. These effects explain some of the anti-inflammatory and antifibrotic properties of Ac-SDKP in hypertension. macrophages; inflammation; activation; angiotensin II HYPERTENSION LEADS TO CARDIAC, renal, and vascular damage. The mechanisms of target organ damage have not been fully elucidated. There is evidence that inflammation contributes to end organ damage (20). We have shown that in ANG IIinduced hypertension (32), as well as in renovascular hypertension (25, 35), mineralocorticoid-salt hypertension (26, 28), spontaneously hypertensive rats (9), and heart failure postmyocardial infarction (24), N-acetyl-seryl-aspartyl-lysyl-proline

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“…Evidence suggested that SAPK/JNK activation was involved in the preconditioning effects 1 . Prevention of left ventricle (LV) dysfunction and remodeling in the mice with cardiomyocyte-targeted expression of MCP-1 was found to involve enhanced neovascularization and promotion of differentiation of cardiac fibroblasts into myofibroblasts 2 . Brain preconditioning by inflammatory inducer has also been reported [3][4][5] .…”

Section: Introductionmentioning

confidence: 99%

“…This protection is called preconditioning, a phenomenon which brief episodes of a sublethal insult induce robust protection against subsequent lethal injuries. For example, cardiomyocyte-targeted expression of monocyte chemotactic protein-1 (MCP-1) showed such a preconditioning protective effect against experimental myocardial ischemic injury 1,2 . Coronary occlusion followed by reperfusion showed that the animals expressing MCP-1 had a much smaller infarct size when compared to the wild type 1 .…”

Section: Introductionmentioning

confidence: 99%

MCPIP mediates preconditioning protection against ischemia

Kolattukudy¹

2016

J Neurol Neuromedicine

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Inflammatory response represents one of the first immune processes following injury. However, evidence indicates that inflammatory response can also induce cellular protection associated in with preconditioning, a phenomenon in which brief episodes of a sublethal insult induce robust protection against subsequent lethal injuries. The elucidation of mechanisms that allow inflammatory response to confer cellular protection is critical to developing new therapeutic strategies against acute ischemic insults. In the present review, we will give a short overview on a novel zinc-finger protein, MCPIP (also known as Zc3h12a or Regnase-1), which may function as a master integrator of endogenous cellular protection exerted by preconditioning.

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Cardiac Overexpression of Monocyte Chemoattractant Protein-1 in Transgenic Mice Prevents Cardiac Dysfunction and Remodeling After Myocardial Infarction

Cited by 138 publications

References 33 publications

Macrophages are required for neonatal heart regeneration

Macrophages are required for neonatal heart regeneration

Novel anti-inflammatory mechanisms ofN-Acetyl-Ser-Asp-Lys-Pro in hypertension-induced target organ damage

MCPIP mediates preconditioning protection against ischemia

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