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30 results on '"Diwan, Abhinav"'

1. The Case for Restoring Organelles to Treat Ischemic Cardiomyopathy: Is DEPP1 an Attractive Target?

Author

Diwan, Abhinav

Subjects
*CELL physiology, *ENDOPLASMIC reticulum, *CYTOLOGY, *PEROXISOMES, *TRANSCRIPTION factors, *REPERFUSION injury, *HEART failure
Abstract

The article explores the potential use of restoring organelles to treat ischemic cardiomyopathy, a common cause of heart failure. The authors focus on the protein DEPP1, which is found in high levels in patients with ischemic cardiomyopathy. They demonstrate that DEPP1 plays a role in myocardial remodeling and cellular pathology caused by sustained cardiomyocyte HIF activation. The authors propose that targeting DEPP1 could improve outcomes in ischemic cardiomyopathy by restoring organelle function. However, more research is needed to fully understand the mechanisms and potential benefits of inhibiting autophagy in this context. The article also discusses the role of HIF signaling in mitophagy and pexophagy, processes that remove damaged mitochondria and peroxisomes from cells. The proteins BNIP3 and NIX are identified as important factors in these processes. The article suggests that restoring the function of mitochondria and peroxisomes may be a promising approach for treating ischemic cardiomyopathy, but further research is necessary to develop targeted therapies and fully comprehend the underlying mechanisms. [Extracted from the article]

Published
2024
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4. Fine-Tuning Cardiac Insulin-Like Growth Factor 1 Receptor Signaling to Promote Health and Longevity.

Author

Abdellatif, Mahmoud, Trummer-Herbst, Viktoria, Heberle, Alexander Martin, Humnig, Alina, Pendl, Tobias, Durand, Sylvère, Cerrato, Giulia, Hofer, Sebastian J., Islam, Moydul, Voglhuber, Julia, Ramos Pittol, José Miguel, Kepp, Oliver, Hoefler, Gerald, Schmidt, Albrecht, Rainer, Peter P., Scherr, Daniel, von Lewinski, Dirk, Bisping, Egbert, McMullen, Julie R., and Diwan, Abhinav

Published
2022
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7. Impaired Protein Quality Control During Left Ventricular Remodeling in Mice With Cardiac Restricted Overexpression of Tumor Necrosis Factor.

Author

Hartupee, Justin, Szalai, Gabor D., Wei Wang, Xiucui Ma, Diwan, Abhinav, and Mann, Douglas L.

Abstract

BACKGROUND: Sustained inflammation in the heart is sufficient to provoke left ventricular dysfunction and left ventricular remodeling. Although inflammation has been linked to many of the biological changes responsible for adverse left ventricular remodeling, the relationship between inflammation and protein quality control in the heart is not well understood. METHODS AND RESULTS: To study the relationship between chronic inflammation and protein quality control, we used a mouse model of dilated cardiomyopathy driven by cardiac restricted overexpression of TNF (tumor necrosis factor; Myh6-sTNF). Myh6-sTNF mice develop protein aggregates containing ubiquitin-tagged proteins within cardiac myocytes related to proteasome dysfunction and impaired autophagy. The 26S proteasome was dysfunctional despite normal function of the core 20S subunit. We found an accumulation of autophagy substrates in Myh6- sTNF mice, which were also seen in tissue from patients with end-stage heart failure. Moreover, there was evidence of impaired autophagosome clearance after chloroquine administration in these mice indicative of impaired autophagic flux. Finally, there was increased mammalian target of rapamycin complex 1 (mTORC1) activation, which has been linked to inhibition of both the proteasome and autophagy. CONCLUSIONS: Myh6-sTNF mice with sustained inflammatory signaling develop proteasome dysfunction and impaired autophagic flux that is associated with enhanced mTORC1 activation. [ABSTRACT FROM AUTHOR]

Published
2017
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9. Tumor Necrosis Factor Receptor-Associated Factor 2 Signaling Provokes Adverse Cardiac Remodeling in the Adult Mammalian Heart.

Author

Divakaran, Vijay G., Evans, Sarah, Topkara, Veli K., Diwan, Abhinav, Burchfield, Jana, Gao, Feng, Dong, Jianwen, Tzeng, Huei-Ping, Sivasubramanian, Natarajan, Barger, Philip M., and Mann, Douglas L.

Abstract

Tumor necrosis factor superfamily ligands provoke a dilated cardiac phenotype signal through a common scaffolding protein termed tumor necrosis factor receptor-associated factor 2 (TRAF2); however, virtually nothing is known about TRAF2 signaling in the adult mammalian heart.We generated multiple founder lines of mice with cardiac-restricted overexpression of TRAF2 and characterized the phenotype of mice with higher expression levels of TRAF2 (myosin heavy chain [MHC]-TRAF2HC). MHC-TRAF2HC transgenic mice developed a time-dependent increase in cardiac hypertrophy, left ventricular dilation, and adverse left ventricular remodeling, and a significant decrease in LV+dP/dt and LV-dP/dt when compared with littermate controls (P<0.05 compared with littermate). During the early phases of left ventricular remodeling, there was a significant increase in total matrix metalloproteinase activity that corresponded with a decrease in total myocardial fibrillar collagen content. As the MHC-TRAF2HC mice aged, there was a significant decrease in total matrix metalloproteinase activity accompanied by an increase in total fibrillar collagen content and an increase in myocardial tissue inhibitor of metalloproteinase-1 levels. There was a significant increase in nuclear factor-κB activation at 4 to 12 weeks and jun N-terminal kinases activation at 4 weeks in the MHC-TRAF2HC mice. Transciptional profiling revealed that >95% of the hypertrophic/dilated cardiomyopathy-related genes that were significantly upregulated genes in the MHC-TRAF2HC hearts contained κB elements in their promoters.These results show for the first time that targeted overexpression of TRAF2 is sufficient to mediate adverse cardiac remodeling in the heart. [ABSTRACT FROM AUTHOR]

Published
2013
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12. Receptor-Independent Cardiac Protein Kinase Cα Activation by Calpain-Mediated Truncation of Regulatory Domains.

Author

Min-Young Kang, Yan Zhang, Matkovich, Scot J., Diwan, Abhinav, Chishti, Athar H., and Dorn II, Gerald W.

Subjects
PROTEIN kinases, HEART cells, CALPAIN, PROTEOLYSIS, ISCHEMIA
Abstract

The article discusses research on the activation of receptor-independent cardiac protein kinase (PK)Cs for determining the biochemical and pathophysiological results of calpain-mediated PKCs proteolysis. The study subjected isolated hearts of mice to global ischemia/reperfusion while transgenic mice were created conditionally to determine the consequences of PKCs fragmentation. The study concluded that the production of C-terminal fragment of PKCs in ischemic hearts can occur through receptor-independent mechanism.

Published
2010
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13. MicroRNA-133a Protects Against Myocardial Fibrosis and Modulates Electrical Repolarization Without Affecting Hypertrophy in Pressure-Overloaded Adult Hearts.

Author

Matkovich, Scot J., Wei Wang, Yizheng Tu, Eschenbacher, William H., Dorn, Lisa E., Condorelli, Gianluigi, Diwan, Abhinav, Nerbonne, Jeanne M., and Dorn II, Gerald W.

Subjects
CARDIAC hypertrophy, FIBROSIS, APOPTOSIS, PREVENTION
Abstract

The article presents a study on the importance of restoring MicroRNA (MiR)-133a to be able to regulate cardiac and skeletal muscle differentiation, reduced myocardial fibrosis and cardiomyocyte apoptosis in the U.S. The study intends to prevent the normal downregulation of miR-133a that is induced through the acute hypertrophic stimulus. The findings reveal of the unreliability of the mRNA signature to predict the miR targets.

Published
2010
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14. Reciprocal regulation of myocardial microRNAs and messenger RNA in human cardiomyopathy and reversal of the microRNA signature by biomechanical support.

Author

Matkovich SJ, Van Booven DJ, Youker KA, Torre-Amione G, Diwan A, Eschenbacher WH, Dorn LE, Watson MA, Margulies KB, Dorn GW 2nd, Matkovich, Scot J, Van Booven, Derek J, Youker, Keith A, Torre-Amione, Guillermo, Diwan, Abhinav, Eschenbacher, William H, Dorn, Lisa E, Watson, Mark A, Margulies, Kenneth B, and Dorn, Gerald W 2nd

Published
2009
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22. Loss of Macrophage mTORC2 Drives Atherosclerosis via FoxO1 and IL-1β Signaling.

Author

Zhang X, Evans TD, Chen S, Sergin I, Stitham J, Jeong SJ, Rodriguez-Velez A, Yeh YS, Park A, Jung IH, Diwan A, Schilling JD, Rom O, Yurdagul A, Epelman S, Cho J, Lodhi IJ, Mittendorfer B, and Razani B

Subjects
Mice, Animals, Mechanistic Target of Rapamycin Complex 2, Macrophages metabolism, Mechanistic Target of Rapamycin Complex 1 metabolism, Transcription Factors metabolism, TOR Serine-Threonine Kinases metabolism, Atherosclerosis genetics, Atherosclerosis metabolism
Abstract

Background: The mTOR (mechanistic target of rapamycin) pathway is a complex signaling cascade that regulates cellular growth, proliferation, metabolism, and survival. Although activation of mTOR signaling has been linked to atherosclerosis, its direct role in lesion progression and in plaque macrophages remains poorly understood. We previously demonstrated that mTORC1 (mTOR complex 1) activation promotes atherogenesis through inhibition of autophagy and increased apoptosis in macrophages., Methods: Using macrophage-specific Rictor- and mTOR-deficient mice, we now dissect the distinct functions of mTORC2 pathways in atherogenesis., Results: In contrast to the atheroprotective effect seen with blockade of macrophage mTORC1, macrophage-specific mTORC2-deficient mice exhibit an atherogenic phenotype, with larger, more complex lesions and increased cell death. In cultured macrophages, we show that mTORC2 signaling inhibits the FoxO1 (forkhead box protein O1) transcription factor, leading to suppression of proinflammatory pathways, especially the inflammasome/IL (interleukin)-1β response, a key mediator of vascular inflammation and atherosclerosis. In addition, administration of FoxO1 inhibitors efficiently rescued the proinflammatory response caused by mTORC2 deficiency both in vitro and in vivo. Interestingly, collective deletion of macrophage mTOR, which ablates mTORC1- and mTORC2-dependent pathways, leads to minimal change in plaque size or complexity, reflecting the balanced yet opposing roles of these signaling arms., Conclusions: Our data provide the first mechanistic details of macrophage mTOR signaling in atherosclerosis and suggest that therapeutic measures aimed at modulating mTOR need to account for its dichotomous functions., Competing Interests: Disclosures None.

Published
2023
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23. Tumor necrosis factor receptor-associated factor 2 mediates mitochondrial autophagy.

Author

Yang KC, Ma X, Liu H, Murphy J, Barger PM, Mann DL, and Diwan A

Subjects
Animals, Animals, Newborn, Disease Models, Animal, Male, Mice, Mice, Inbred C57BL, Mitochondria, Heart pathology, Myocardial Reperfusion Injury pathology, Myocytes, Cardiac pathology, Rats, Signal Transduction, Autophagy, Mitochondria, Heart metabolism, Myocardial Reperfusion Injury metabolism, Myocytes, Cardiac metabolism, TNF Receptor-Associated Factor 2 metabolism
Abstract

Background: Tumor necrosis factor (TNF) signaling protects against ischemia/reperfusion-induced cardiomyocyte death, in vitro, ex vivo, and in vivo. TNF-receptor-associated factor 2 (TRAF2), an E3 ubiquitin ligase, coordinates cytoprotective signaling downstream of both TNF receptors, via unclear mechanisms. Noting that TRAF2 is recruited to mitochondria, and that autophagic removal of ubiquitin-tagged damaged mitochondria is cytoprotective, we tested the hypothesis that TRAF2 mediates mitochondrial autophagy., Methods and Results: TRAF2 localizes to the mitochondria in neonatal rat cardiac myocytes, and TNF treatment transcriptionally upregulates TRAF2 abundance in the mitochondrial subfraction. TRAF2 colocalizes with ubiquitin, p62 adaptor protein, and mitochondria within LC3-bound autophagosomes; and exogenous TRAF2 enhances autophagic removal of mitochondria. TRAF2 knockdown with adenoviral shRNA transduction induces accumulation of depolarized mitochondria in resting neonatal rat cardiac myocytes, as well as in those treated with TNF or uncoupling agent carbonyl cyanide m-chlorophenyl hydrazone, suggesting an essential role for TRAF2 in homeostatic and stress-induced mitochondrial autophagy. TRAF2 also colocalizes and interacts with PARKIN, a previously described E3 ubiquitin ligase and mitophagy effector, on depolarized mitochondria in neonatal rat cardiac myocytes. Exogenous expression of TRAF2, but not its E3 ligase-deficient mutants, is sufficient to partially restore mitophagy in the setting of PARKIN knockdown, suggesting redundancy in their ubiquitin ligase roles. TRAF2 abundance increases in the mitochondrial subfraction of ischemia/reperfusion-modeled hearts; and exogenous TRAF2, but not its E3 ligase-deficient mutants, reduces depolarized mitochondria and rescues cell death in neonatal rat cardiac myocytes subjected to hypoxia/reoxygenation., Conclusions: Taken together, these data indicate an essential role for TRAF2 in concert with PARKIN as a mitophagy effector, which contributes to TRAF2-induced cytoprotective signaling., (© 2014 American Heart Association, Inc.)

Published
2015
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24. Induction of lysosomal biogenesis in atherosclerotic macrophages can rescue lipid-induced lysosomal dysfunction and downstream sequelae.

Author

Emanuel R, Sergin I, Bhattacharya S, Turner J, Epelman S, Settembre C, Diwan A, Ballabio A, and Razani B

Subjects
Animals, Apolipoproteins E deficiency, Atherosclerosis pathology, Autophagy, Autophagy-Related Protein 5, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors, Cell Membrane Permeability, Chloroquine pharmacology, Cholesterol metabolism, Hydrogen-Ion Concentration, Inclusion Bodies metabolism, Inflammasomes metabolism, Interleukin-1beta metabolism, Lipids, Lipoproteins, LDL metabolism, Lysosomes drug effects, Mice, Mice, Inbred C57BL, Mice, Transgenic, Microtubule-Associated Proteins deficiency, Microtubule-Associated Proteins genetics, Plaque, Atherosclerotic metabolism, Plaque, Atherosclerotic pathology, Polyubiquitin metabolism, Proteolysis, Sterol Esterase metabolism, Transcription, Genetic, Atherosclerosis metabolism, Lysosomes physiology, Macrophages, Peritoneal physiology
Abstract

Objective: Recent reports of a proatherogenic phenotype in mice with macrophage-specific autophagy deficiency have renewed interest in the role of the autophagy-lysosomal system in atherosclerosis. Lysosomes have the unique ability to process both exogenous material, including lipids and autophagy-derived cargo such as dysfunctional proteins/organelles. We aimed to understand the effects of an atherogenic lipid environment on macrophage lysosomes and to evaluate novel ways to modulate this system., Approach and Results: Using a variety of complementary techniques, we show that oxidized low-density lipoproteins and cholesterol crystals, commonly encountered lipid species in atherosclerosis, lead to profound lysosomal dysfunction in cultured macrophages. Disruptions in lysosomal pH, proteolytic capacity, membrane integrity, and morphology are readily seen. Using flow cytometry, we find that macrophages isolated from atherosclerotic plaques also display features of lysosome dysfunction. We then investigated whether enhancing lysosomal function can be beneficial. Transcription factor EB (TFEB) is the only known transcription factor that is a master regulator of lysosomal biogenesis although its role in macrophages has not been studied. Lysosomal stress induced by chloroquine or atherogenic lipids leads to TFEB nuclear translocation and activation of lysosomal and autophagy genes. TFEB overexpression in macrophages further augments this prodegradative response and rescues several deleterious effects seen with atherogenic lipid loading as evidenced by blunted lysosomal dysfunction, reduced secretion of the proinflammatory cytokine interleukin-1β, enhanced cholesterol efflux, and decreased polyubiquitinated protein aggregation., Conclusions: Taken together, these data demonstrate that lysosomal function is markedly impaired in atherosclerosis and suggest that induction of a lysosomal biogenesis program in macrophages has antiatherogenic effects., (© 2014 American Heart Association, Inc.)

Published
2014
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25. Receptor-independent cardiac protein kinase Calpha activation by calpain-mediated truncation of regulatory domains.

Author

Kang MY, Zhang Y, Matkovich SJ, Diwan A, Chishti AH, and Dorn GW 2nd

Subjects
Animals, Calcium metabolism, Cardiomyopathies pathology, Carrier Proteins metabolism, Humans, Mice, Mice, Transgenic, Myocardial Infarction metabolism, Myocardial Infarction pathology, Myocardial Reperfusion Injury pathology, Myocardium pathology, Phosphorylation physiology, Protein Kinase C-alpha chemistry, Protein Kinase C-alpha genetics, Protein Serine-Threonine Kinases chemistry, Protein Serine-Threonine Kinases genetics, Protein Serine-Threonine Kinases metabolism, Protein Structure, Tertiary, Signal Transduction physiology, Calpain metabolism, Cardiomyopathies metabolism, Myocardial Reperfusion Injury metabolism, Myocardium metabolism, Protein Kinase C-alpha metabolism
Abstract

Rationale: Protein kinase (PK)Cs and calpain cysteine proteases are highly expressed in myocardium. Ischemia produces calcium overload that activates calpains and conventional PKCs. However, calpains can proteolytically process PKCs, and the potential in vivo consequences of this interaction are unknown., Objective: To determine the biochemical and pathophysiological consequences of calpain-mediated cardiac PKCα proteolysis., Methods and Results: Isolated mouse hearts subjected to global ischemia/reperfusion demonstrated cleavage of PKCα. Calpain 1 overexpression was not sufficient to produce PKCα cleavage in normal hearts, but ischemia-induced myocardial PKCα cleavage and myocardial injury were greatly increased by cardiac-specific expression of calpain 1. In contrast, calpain 1 gene ablation or inhibition with calpastatin prevented ischemia/reperfusion induced PKCα cleavage; infarct size was decreased and ventricular function enhanced in infarcted calpain 1 knockout hearts. To determine consequences of PKCα fragmentation on myocardial protein phosphorylation, transgenic mice were created conditionally expressing full-length PKCα or its N-terminal and C-terminal calpain 1 cleavage fragments. Two-dimensional mapping of ventricular protein extracts showed a distinct PKCα phosphorylation profile that was exaggerated and distorted in hearts expressing the PKCα C-terminal fragment. MALDI mass spectroscopy revealed hyperphosphorylation of myosin-binding protein C and phosphorylation of atypical substrates by the PKCα C-terminal fragment. Expression of parent PKCα produced a mild cardiomyopathy, whereas myocardial expression of the C-terminal PKCα fragment induced a disproportionately severe, rapidly lethal cardiomyopathy., Conclusions: Proteolytic processing of PKCα by calcium-activated calpain activates pathological cardiac signaling through generation of an unregulated and/or mistargeted kinase. Production of the PKCα C-terminal fragment in ischemic hearts occurs via a receptor-independent mechanism.

Published
2010
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26. Sarcoplasmic reticulum calcium overloading in junctin deficiency enhances cardiac contractility but increases ventricular automaticity.

Author

Yuan Q, Fan GC, Dong M, Altschafl B, Diwan A, Ren X, Hahn HH, Zhao W, Waggoner JR, Jones LR, Jones WK, Bers DM, Dorn GW 2nd, Wang HS, Valdivia HH, Chu G, and Kranias EG

Subjects
Animals, Arrhythmias, Cardiac chemically induced, Arrhythmias, Cardiac physiopathology, Cardiotonic Agents, Electrocardiography, Embryonic Stem Cells, Female, Gene Expression Regulation physiology, Homeostasis physiology, Isoproterenol, Male, Mice, Mice, Knockout, Myocardial Contraction genetics, Myocytes, Cardiac physiology, Patch-Clamp Techniques, Signal Transduction physiology, Ventricular Dysfunction etiology, Ventricular Dysfunction genetics, Calcium metabolism, Calcium-Binding Proteins genetics, Calcium-Binding Proteins metabolism, Membrane Proteins genetics, Membrane Proteins metabolism, Mixed Function Oxygenases genetics, Mixed Function Oxygenases metabolism, Muscle Proteins genetics, Muscle Proteins metabolism, Myocardial Contraction physiology, Sarcoplasmic Reticulum metabolism, Ventricular Dysfunction physiopathology
Abstract

Background: Abnormal sarcoplasmic reticulum calcium (Ca) cycling is increasingly recognized as an important mechanism for increased ventricular automaticity that leads to lethal ventricular arrhythmias. Previous studies have linked lethal familial arrhythmogenic disorders to mutations in the ryanodine receptor and calsequestrin genes, which interact with junctin and triadin to form a macromolecular Ca-signaling complex. The essential physiological effects of junctin and its potential regulatory roles in sarcoplasmic reticulum Ca cycling and Ca-dependent cardiac functions, such as myocyte contractility and automaticity, are unknown., Methods and Results: The junctin gene was targeted in embryonic stem cells, and a junctin-deficient mouse was generated. Ablation of junctin was associated with enhanced cardiac function in vivo, and junctin-deficient cardiomyocytes exhibited increased contractile and Ca-cycling parameters. Short-term isoproterenol stimulation elicited arrhythmias, including premature ventricular contractions, atrioventricular heart block, and ventricular tachycardia. Long-term isoproterenol infusion also induced premature ventricular contractions and atrioventricular heart block in junctin-null mice. Further examination of the electrical activity revealed a significant increase in the occurrence of delayed afterdepolarizations. Consistently, 25% of the junctin-null mice died by 3 months of age with structurally normal hearts., Conclusions: Junctin is an essential regulator of sarcoplasmic reticulum Ca release and contractility in normal hearts. Ablation of junctin is associated with aberrant Ca homeostasis, which leads to fatal arrhythmias. Thus, normal intracellular Ca cycling relies on maintenance of junctin levels and an intricate balance among the components in the sarcoplasmic reticulum quaternary Ca-signaling complex.

Published
2007
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27. Cardiac-specific ablation of G-protein receptor kinase 2 redefines its roles in heart development and beta-adrenergic signaling.

Author

Matkovich SJ, Diwan A, Klanke JL, Hammer DJ, Marreez Y, Odley AM, Brunskill EW, Koch WJ, Schwartz RJ, and Dorn GW 2nd

Subjects
Adrenergic beta-Agonists toxicity, Animals, Cardiomyopathies chemically induced, Cardiotonic Agents pharmacology, Embryonic Development, G-Protein-Coupled Receptor Kinase 2, Gene Targeting, Genes, Lethal, Isoproterenol toxicity, Mice, Signal Transduction, Tachyphylaxis, beta-Adrenergic Receptor Kinases genetics, Adrenergic beta-Agonists pharmacology, Heart embryology, Myocytes, Cardiac enzymology, beta-Adrenergic Receptor Kinases physiology
Abstract

G-protein receptor kinase 2 (GRK2) is 1 of 7 mammalian GRKs that phosphorylate ligand-bound 7-transmembrane receptors, causing receptor uncoupling from G proteins and potentially activating non-G-protein signaling pathways. GRK2 is unique among members of the GRK family in that its genetic ablation causes embryonic lethality. Cardiac abnormalities in GRK2 null embryos implicated GRK2 in cardiac development but prevented studies of the knockout phenotype in adult hearts. Here, we created GRK2-loxP-targeted mice and used Cre recombination to generate germline and cardiac-specific GRK2 knockouts. GRK2 deletion in the preimplantation embryo with EIIa-Cre (germline null) resulted in developmental retardation and embryonic lethality between embryonic day 10.5 (E10.5) and E11.5. At E9.5, cardiac myocyte specification and cardiac looping were normal, but ventricular development was delayed. Cardiomyocyte-specific ablation of GRK2 in the embryo with Nkx2.5-driven Cre (cardiac-specific GRK2 knockout) produced viable mice with normal heart structure, function, and cardiac gene expression. Cardiac-specific GRK2 knockout mice exhibited enhanced inotropic sensitivity to the beta-adrenergic receptor agonist isoproterenol, with impairment of normal inotropic and lusitropic tachyphylaxis, and exhibited accelerated development of catecholamine toxicity with chronic isoproterenol treatment. These findings show that cardiomyocyte autonomous GRK2 is not essential for myocardial development after cardiac specification, suggesting that embryonic developmental abnormalities may be attributable to extracardiac effects of GRK2 ablation. In the adult heart, cardiac GRK2 is a major factor regulating inotropic and lusitropic tachyphylaxis to beta-adrenergic agonist, which likely contributes to its protective effects in catecholamine cardiomyopathy.

Published
2006
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28. Targeted overexpression of noncleavable and secreted forms of tumor necrosis factor provokes disparate cardiac phenotypes.

Author

Diwan A, Dibbs Z, Nemoto S, DeFreitas G, Carabello BA, Sivasubramanian N, Wilson EM, Spinale FG, and Mann DL

Subjects
Animals, Fibrillar Collagens analysis, Gene Expression Regulation, Gene Targeting, Hypertrophy, Left Ventricular metabolism, Hypertrophy, Left Ventricular pathology, Kinetics, Matrix Metalloproteinase Inhibitors, Matrix Metalloproteinases metabolism, Mice, Mice, Transgenic, Mutation, Myocardium chemistry, Myocardium pathology, Myocardium ultrastructure, Phenotype, Tissue Inhibitor of Metalloproteinases metabolism, Tumor Necrosis Factor-alpha metabolism, Hypertrophy, Left Ventricular etiology, Tumor Necrosis Factor-alpha genetics, Ventricular Remodeling
Abstract

Background: Recent studies suggest that posttranslation processing or "shedding" (ie, secretion) of tumor necrosis factor (TNF) by tumor necrosis factor-alpha converting enzyme (TACE) may contribute to the left ventricular (LV) remodeling that occurs in the failing human heart., Methods and Results: To address the functional significance of TNF shedding, we generated lines of transgenic mice with targeted overexpression of secreted wild-type (MHCsTNF2) TNF and overexpression of a mutated noncleavable transmembrane form of TNF (MHCmTNF). Both lines of mice had overlapping levels of myocardial TNF protein; however, the phenotypes of the MHCsTNF2 and MHCmTNF mice were strikingly disparate. Whereas the MHCmTNF mice developed a concentric LV hypertrophy phenotype, the MHCsTNF2 mice developed a dilated LV phenotype. The fibrillar collagen weave in MHCmTNF mice with concentric hypertrophy was characterized by thick collagen fibrils and increased collagen content, whereas the fibrillar collagen weave in the MHCsTNF2 mice with LV dilation was characterized by a diminished collagen content. Inhibition of matrix metalloproteinases with a broad-based matrix metalloproteinase inhibitor prevented LV dilation in the MHCsTNF2 mice., Conclusions: These findings suggest that posttranslational processing of TNF, as opposed to TNF expression per se, is responsible for the adverse cardiac remodeling that occurs after sustained TNF overexpression.

Published
2004
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29. Targeted overexpression of transmembrane tumor necrosis factor provokes a concentric cardiac hypertrophic phenotype.

Author

Dibbs ZI, Diwan A, Nemoto S, DeFreitas G, Abdellatif M, Carabello BA, Spinale FG, Feuerstein G, Sivasubramanian N, and Mann DL

Subjects
ADAM Proteins, ADAM17 Protein, Animals, Animals, Genetically Modified, Cardiomegaly genetics, Cardiomegaly pathology, Cats, Disease Models, Animal, Disease Progression, Enzyme Inhibitors pharmacology, Metalloendopeptidases antagonists & inhibitors, Mice, Mice, Transgenic, Myocardium pathology, Organ Specificity genetics, Phenotype, RNA, Messenger metabolism, Survival Analysis, Transgenes, Tumor Necrosis Factor-alpha genetics, Cardiomegaly metabolism, Cell Membrane metabolism, Gene Expression Regulation, Developmental, Gene Targeting methods, Myocardium metabolism, Tumor Necrosis Factor-alpha biosynthesis
Abstract

Background: Tumor necrosis factor (TNF) is initially synthesized as a 26-kDa transmembrane protein that is enzymatically cleaved by TNF-alpha converting enzyme (TACE) to generate a 17-kDa form of "secreted" TNF. Whereas the effects of secreted TNF in the heart have been characterized extensively, the effects of transmembrane TNF in the heart are unknown., Methods and Results: We generated lines of transgenic mice with cardiac-restricted overexpression of a noncleavable, transmembrane form of TNF. We next treated a previously generated transgenic line of mice with cardiac-restricted expression of cleavable TNF (referred to as MHCsTNF mice) with a TACE inhibitor (DPC-IDR1) to determine whether TACE inhibition would prevent the transition from concentric hypertrophy to left ventricular (LV) dilation that occurs in this line of transgenic mice. Two of the founder lines did not have a demonstrable phenotype (M-41 and M-45), whereas a third line developed a concentric hypertrophic cardiac phenotype (M-48). Characterization of the M-48 line at 6 weeks of age showed that this line developed concentric hypertrophy, with an increase in myocyte cross-sectional area and reexpression of the fetal gene program. Four weeks of TACE inhibition abrogated the LV dilation in the MHCsTNF mice and resulted in an increase in LV wall thickness and increased myocyte cross-sectional area, thus mimicking the effects observed in the mice with noncleavable, transmembrane TNF., Conclusions: These studies show that transmembrane TNF is biologically active and provokes a concentric hypertrophic cardiac phenotype, thus suggesting that posttranslational processing (ie, secretion) of TNF is responsible for the dilated cardiomyopathic phenotype in mice with targeted, cardiac-restricted overexpression of TNF.

Published
2003
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30. Activation and functional significance of the renin-angiotensin system in mice with cardiac restricted overexpression of tumor necrosis factor.

Author

Flesch M, Höper A, Dell'Italia L, Evans K, Bond R, Peshock R, Diwan A, Brinsa TA, Wei CC, Sivasubramanian N, Spinale FG, and Mann DL

Subjects
Age Factors, Angiotensin I metabolism, Angiotensin II metabolism, Angiotensin Receptor Antagonists, Angiotensinogen biosynthesis, Angiotensinogen genetics, Animals, Body Weight drug effects, Body Weight genetics, Cardiomegaly drug therapy, Cardiomegaly metabolism, Collagen metabolism, Hemodynamics drug effects, Losartan pharmacology, Mice, Mice, Transgenic, Organ Size drug effects, Organ Size genetics, Organ Specificity, Peptidyl-Dipeptidase A genetics, Peptidyl-Dipeptidase A metabolism, RNA, Messenger metabolism, Receptor, Angiotensin, Type 1, Receptor, Angiotensin, Type 2, Receptors, Angiotensin genetics, Receptors, Angiotensin metabolism, Renin biosynthesis, Renin genetics, Renin-Angiotensin System drug effects, Renin-Angiotensin System genetics, Ventricular Remodeling drug effects, Ventricular Remodeling physiology, Cardiomegaly genetics, Myocardium metabolism, Renin-Angiotensin System physiology, Tumor Necrosis Factor-alpha biosynthesis, Tumor Necrosis Factor-alpha genetics
Abstract

Background: The functional significance of cross-regulation between the renin-angiotensin system (RAS) and tumor necrosis factor (TNF) has been established in nonmyocyte cell types; however, the degree and functional significance of the interaction between RAS and TNF has not been characterized in the heart., Methods and Results: We examined the expression of components of the RAS in a line of transgenic mice (MHCsTNF) with cardiac restricted overexpression of TNF. When examined at 4, 8, and 12 weeks of age, the MHCsTNF mice had increased activation of myocardial RAS, as shown by an increase in ACE mRNA level and ACE activity and increased angiotensin II peptide levels. Furthermore, myocardial angiotensin receptor mRNA and protein levels were reduced in the MHCsTNF mice, consistent with homologous desensitization of the receptors. However, expression of renin and angiotensinogen was not increased in MHCsTNF mice compared with littermate controls. To determine the functional significance of RAS activation in the MHCsTNF mice, we treated the mice with an angiotensin type I receptor antagonist, losartan (30 mg/kg), or diluent from 4 to 8 weeks of age. Analysis of cardiac structure with MRI showed that treatment with losartan normalized left ventricular mass and wall thickness. Furthermore, treatment with losartan reduced myocardial collagen content and reduced the incidence of myocyte apoptosis., Conclusions: Taken together, these results show that there are functionally significant interactions between RAS and TNF in the heart and that these interactions play an important role in the development and progression of left ventricular remodeling.

Published
2003
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