Cardiomyopathy and Worsened Ischemic Heart Failure in SM22-α Cre-Mediated Neuropilin-1 Null Mice

Wang, Ying; Yamada, Satsuki; Thirunavukkarasu, Mahesh; Nin, Verónica; Joshi, Mandip; Rishi, Muhammed T.; Bhattacharya, Santanu; Camacho-Pereira, Juliana; Sharma, Anil Kumar; Shameer, Khader; Kocher, Jean-Pierre A.; Sánchez, Juan A.; Wang, Enfeng; Hoeppner, Luke H.; Dutta, Shamit K.; Leof, Edward B.; Shah, Vijay H.; Claffey, Kevin P.; Chini, Eduardo N.; Simons, Michael; Terzic, André; Maulik, Nilanjana; Mukhopadhyay, Debabrata

doi:10.1161/atvbaha.115.305566

Cited by 43 publications

(58 citation statements)

References 59 publications

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“…These include IL-10 and decorin that ameliorates high fat diet-induced cardiac dysfunction [29, 37], neuropilin that attenuates cardiomyopathy [38], and LIX (CXCL-5) that has a protective role in coronary artery disease [39]; see Figure 4. Other suppressed anti-inflammatory markers in the hearts of ZO-C include interferon- γ (IFN- γ ) that has cardioprotective roles and Platelet Derived Growth Factor (PDGF AA) that improves wound healing [40, 41].…”

Section: Resultsmentioning

confidence: 99%

Differential Regulation of Cardiac Function and Intracardiac Cytokines by Rapamycin in Healthy and Diabetic Rats

Lück

DeMarco

Mahmood

et al. 2017

Oxidative Medicine and Cellular Longevity

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Diabetes is comorbid with cardiovascular disease and impaired immunity. Rapamycin improves cardiac functions and extends lifespan by inhibiting the mechanistic target of rapamycin complex 1 (mTORC1). However, in diabetic murine models, Rapamycin elevates hyperglycemia and reduces longevity. Since Rapamycin is an immunosuppressant, we examined whether Rapamycin (750 μg/kg/day) modulates intracardiac cytokines, which affect the cardiac immune response, and cardiac function in male lean (ZL) and diabetic obese Zucker (ZO) rats. Rapamycin suppressed levels of fasting triglycerides, insulin, and uric acid in ZO but increased glucose. Although Rapamycin improved multiple diastolic parameters (E/E′, E′/A′, E/Vp) initially, these improvements were reversed or absent in ZO at the end of treatment, despite suppression of cardiac fibrosis and phosphoSer473Akt. Intracardiac cytokine protein profiling and Ingenuity® Pathway Analysis indicated suppression of intracardiac immune defense in ZO, in response to Rapamycin treatment in both ZO and ZL. Rapamycin increased fibrosis in ZL without increasing phosphoSer473Akt and differentially modulated anti-fibrotic IL-10, IFNγ, and GM-CSF in ZL and ZO. Therefore, fundamental difference in intracardiac host defense between diabetic ZO and healthy ZL, combined with differential regulation of intracardiac cytokines by Rapamycin in ZO and ZL hearts, underlies differential cardiac outcomes of Rapamycin treatment in health and diabetes.

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Section: Resultsmentioning

confidence: 99%

Differential Regulation of Cardiac Function and Intracardiac Cytokines by Rapamycin in Healthy and Diabetic Rats

Lück

DeMarco

Mahmood

et al. 2017

Oxidative Medicine and Cellular Longevity

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“…All experiments involving animals were approved by The University of Edinburgh Animal Welfare and Ethical Review Body and by the Unite Kingdom Home Office. Experiments used adult male (10–14 wk of age) mice with global deficiency on a C57Bl/6 genetic background ( Hsd11b1 −/− ) ( 8 , 20 ), with C57Bl/6 controls, or mice in which deletion was targeted to vascular smooth muscle and cardiomyocytes ( 21 , 22 ). These Hsd11b1 fl/fl Sm22 α -Cre + ( Hsd11b1 CVCre+ ) were generated by crossing Sm22 α -Cre mice with Hsd11b1 fl/fl mice, homozygous for a “floxed” allele of Hsd11b1 (generated by Artemis Pharmaceuticals directly onto a C57BL/6J background).…”

Section: Methodsmentioning

confidence: 99%

Cardiomyocyte and Vascular Smooth Muscle-Independent 11β-Hydroxysteroid Dehydrogenase 1 Amplifies Infarct Expansion, Hypertrophy, and the Development of Heart Failure After Myocardial Infarction in Male Mice

et al. 2016

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Global deficiency of 11β-hydroxysteroid dehydrogenase type 1 (11β-HSD1), an enzyme that regenerates glucocorticoids within cells, promotes angiogenesis, and reduces acute infarct expansion after myocardial infarction (MI), suggesting that 11β-HSD1 activity has an adverse influence on wound healing in the heart after MI. The present study investigated whether 11β-HSD1 deficiency could prevent the development of heart failure after MI and examined whether 11β-HSD1 deficiency in cardiomyocytes and vascular smooth muscle cells confers this protection. Male mice with global deficiency in 11β-HSD1, or with Hsd11b1 disruption in cardiac and vascular smooth muscle (via SM22α-Cre recombinase), underwent coronary artery ligation for induction of MI. Acute injury was equivalent in all groups. However, by 8 weeks after induction of MI, relative to C57Bl/6 wild type, globally 11β-HSD1-deficient mice had reduced infarct size (34.7 ± 2.1% left ventricle [LV] vs 44.0 ± 3.3% LV, P = .02), improved function (ejection fraction, 33.5 ± 2.5% vs 24.7 ± 2.5%, P = .03) and reduced ventricular dilation (LV end-diastolic volume, 0.17 ± 0.01 vs 0.21 ± 0.01 mL, P = .01). This was accompanied by a reduction in hypertrophy, pulmonary edema, and in the expression of genes encoding atrial natriuretic peptide and β-myosin heavy chain. None of these outcomes, nor promotion of periinfarct angiogenesis during infarct repair, were recapitulated when 11β-HSD1 deficiency was restricted to cardiac and vascular smooth muscle. 11β-HSD1 expressed in cells other than cardiomyocytes or vascular smooth muscle limits angiogenesis and promotes infarct expansion with adverse ventricular remodeling after MI. Early pharmacological inhibition of 11β-HSD1 may offer a new therapeutic approach to prevent heart failure associated with ischemic heart disease.

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“…One theory is that excess mitochondrial activity and ROS production is responsible in part for cardiomyopathy and sudden cardiac death due to arrhythmia. 60 This concept is supported by a recent study by Wang and colleagues in ATVB , 61 demonstrating that mice deficient in neuropilin-1 in cardiomyocytes and smooth muscle cells exhibited cardiomyopathy associated with increased mitochondrial content and aggravated ischemia-induced heart failure. Thus, neurpilin-1, a receptor that binds several structurally distinct ligands, including VEGF and TGF-β, maintains mitochondrial homeostasis in the failing heart.…”

Section: Metabolic Flexibility and Dysfunction In Cardiac Cellsmentioning

confidence: 82%

Metabolic Flexibility and Dysfunction in Cardiovascular Cells

Vallerie

Bornfeldt

2015

ATVB

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Cardiomyopathy and Worsened Ischemic Heart Failure in SM22-α Cre-Mediated Neuropilin-1 Null Mice

Cited by 43 publications

References 59 publications

Differential Regulation of Cardiac Function and Intracardiac Cytokines by Rapamycin in Healthy and Diabetic Rats

Differential Regulation of Cardiac Function and Intracardiac Cytokines by Rapamycin in Healthy and Diabetic Rats

Cardiomyocyte and Vascular Smooth Muscle-Independent 11β-Hydroxysteroid Dehydrogenase 1 Amplifies Infarct Expansion, Hypertrophy, and the Development of Heart Failure After Myocardial Infarction in Male Mice

Metabolic Flexibility and Dysfunction in Cardiovascular Cells

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