Your search keyword '"Chandrasekar Bysani"' showing total 16 results

1. Inhibition of inflammatory response in transgenic fat-1 mice on a calorie-restricted diet

Author

Bhattacharya, Arunabh, Chandrasekar, Bysani, Rahman, Md Mizanur, Banu, Jameela, Kang, Jing X., and Fernandes, Gabriel

Subjects

*CELLULAR immunity, *ANTHROPOMETRY, *MAMMAL body composition, *NUCLEIC acids

Abstract

Abstract: Both n −3 fatty acids (n −3 FA) and calorie-restriction (CR) exert anti-inflammatory effects in animal models of autoimmunity and inflammation. In the present study we investigated the synergistic anti-inflammatory effects of n −3 FA and CR on LPS-mediated inflammatory responses using fat-1 transgenic mice that generate n −3 FA endogenously. Wild-type (WT) and fat-1 mice were maintained on ad libitum (AL) or CR (40% less than AL) diet for 5 mo; splenocytes were cultured in vitro with/without LPS. Our results show: (i) no difference in body weights between WT and fat-1 mice on AL or CR diets, (ii) lower n −6/n −3 FA ratio in splenocytes from fat-1 mice on both AL and CR diets, (iii) significant reduction in NF-κB (p65/p50) and AP-1 (c-Fos/c-Jun) DNA-binding activities in splenocytes from fat-1/CR mice following LPS treatment, and (iv) significant reduction in κB- and AP-1-responsive IL-6 and TNF-α secretion following LPS treatment in splenocytes from fat-1/CR mice. The inhibition of LPS-mediated effects was more pronounced in fat-1/CR mice when compared to fat-1/AL or WT/CR mice. These data show that transgenic expression of fat-1 results in decreased pro-inflammatory n −6 FA, and demonstrate for the first time that splenocytes from fat-1 mice on CR diet exhibit reduced pro-inflammatory response when challenged with LPS. These results suggest that n −3 lipids with moderate CR may confer protection in autoimmune and inflammatory diseases. [Copyright &y& Elsevier]

Published

2006

2. Interleukin-18 induces human cardiac endothelial cell death via a novel signaling pathway involving NF-κB-dependent PTEN activation

Author

Chandrasekar, Bysani, Valente, Anthony J., Freeman, Gregory L., Mahimainathan, Lenin, and Mummidi, Srinivas

Subjects

*APOPTOSIS, *CELL death, *GROWTH factors, *TUMOR suppressor genes

Abstract

Abstract: The tumor suppressor gene PTEN (phosphatase and tensin homologue deleted on chromosome 10) antagonizes the pro-survival signaling of Akt and promotes cell death. Previously, we demonstrated that IL-18 induced apoptosis in human cardiac microvascular endothelial cells (HCMEC). Here we have investigated the role of PTEN in this response. Our results demonstrate that IL-18 reduced phospho-Akt and bcl-2 levels, stimulated NF-κB activation, and induced PTEN-promoter-reporter activity, mRNA expression, and protein levels in HCMEC. IL-18-mediated PTEN transcription was enhanced by ectopic expression of wild type p65, but inhibited by dominant negative (dn) IκB-α, dnp65, and dnIKKβ. Furthermore, overexpression of constitutively active Akt and wild type bcl-2 blocked IL-18-mediated cell death. While forced expression of PTEN potentiated, expression of catalytically inactive PTEN attenuated IL-18-mediated cell death. IL-18-induced activation of NF-κB and PTEN upregulation were mediated by p38MAPK. Together, these studies demonstrate a novel signal transduction pathway involving p38MAPK-NF-κB-PTEN in IL-18-mediated HCMEC death, and identify IL-18 as potential therapeutic target to inhibit or reduce myocardial inflammation and injury. [Copyright &y& Elsevier]

Published

2006

3. β-Adrenergic stimulation induces interleukin-18 expression via β2-AR, PI3K, Akt, IKK, and NF-κB

Author

Chandrasekar, Bysani, Marelli-Berg, Federica M., Tone, Masahide, Bysani, Sailaja, Prabhu, Sumanth D., and Murray, David R.

Subjects

*INTERLEUKINS, *HEART failure, *CYTOKINES, *ISOPROTERENOL

Abstract

We investigated whether β-adrenergic receptor (β-AR) stimulation induces the expression of interleukin (IL)-18, a proinflammatory cytokine, in myocardium and in cardiac-derived endothelial cells (CDEC) via activation of nuclear factor (NF)-κB. Our results indicate that isoproterenol (ISO) activates NF-κB DNA binding activity, and induces myocardial and systemic elaboration of IL-18 via β2-AR signaling. Furthermore, in CDEC, ISO increased basal and inducible promoter activities, increased IL-18 gene transcription and mRNA stability, and induced IL-18 expression via β2-AR agonism. Signaling required Gi, PI3K, Akt, IKK, and NF-κB. In conclusion, our results indicate for the first time that isoproterenol induces myocardial and systemic elaboration of IL-18 via a β2-AR and NF-κB-dependent mechanism. Similar events may occur in heart failure, a disease state characterized by sustained β-AR activation. [Copyright &y& Elsevier]

Published

2004

4. TNF-α and <f>H2O2</f> induce IL-18 and IL-<f>18Rβ</f> expression in cardiomyocytes via NF-<f>κB</f> activation

Author

Chandrasekar, Bysani, Colston, James T., de la Rosa, Sam D., Rao, Perla P., and Freeman, Gregory L.

Subjects

*CORONARY disease, *CYTOKINES

Abstract

Myocardial ischemia/reperfusion is characterized by oxidative stress and induction of proinflammatory cytokines. Interleukin (IL)-18, a member of the IL-1 family, acts as a proinflammatory cytokine, and is induced during various immune and inflammatory disorders. Therefore, in the present study we investigated whether IL-18 expression is regulated by cytokines and oxidative stress in cardiomyocytes. TNF-α induced rapid and sustained activation of NF-κB whereas H2O2 induced delayed and transient activation. Both TNF-α and H2O2 induced IL-18 mRNA and precursor protein in cardiomyocytes, and IL-18 release into culture supernatants. However, only TNF-α led to sustained expression. Expression of IL-18Rβ, but not α, was induced by both agonists. TNF-α and H2O2 induced delayed expression of IL-18 BP. Pretreatment with PDTC attenuated TNF-α and H2O2 induced IL-18 and IL-18Rβ, but not basal expression of IL-18Rα. These results indicate that adult cardiomyocytes express IL-18 and its receptors, and proinflammatory cytokines and oxidative stress regulate their expression via activation of NF-κB. Presence of both ligand and receptors suggests IL-18 impacts myocardial biology through an autocrine pathway. [Copyright &y& Elsevier]

Published

2003

5. Ultrasound-targeted antisense oligonucleotide attenuates ischemia/reperfusion-induced myocardial tumor necrosis factor-alpha

Author

Erikson, John M., Freeman, Gregory L., and Chandrasekar, Bysani

Subjects

*OLIGONUCLEOTIDES, *THERAPEUTICS

Abstract

Ultrasound contrast agents are now emerging as effective vehicles for delivering therapeutic agents to target tissues. In the present study, we used ultrasound-targeted, contrast-bound antisense oligonucleotides to inhibit the expression of tumor necrosis factor-alpha (TNF-α), a proinflammatory cytokine with negative inotropic effects. We compared the efficacy of left ventricular vs. intravenous administration and determined the optimal time for delivery. WKY rats were treated with perfluorocarbon-exposed sonicated dextrose albumin (PESDA) microspheres incubated with 100 μg of antisense oligonucleotide directed against TNF-α. Contrast was infused into either the superior vena cava or the left ventricular cavity along with simultaneous application of ultrasound. Twenty-four hours later, the animals underwent 15 min of ischemia and 2 h reperfusion. Control animals underwent sham operation only, ischemia/reperfusion only, or received PESDA only. A second group received treatment just prior to, or immediately after the onset of ischemia. At the end of the experimental period, hearts were removed and analyzed for TNF-α by northern and western blotting. While no TNF-α expression was detected in sham-operated animals, robust expression of TNF-α mRNA and protein was seen in controls treated with ultrasound and PESDA alone. In contrast, intravenous or left ventricular administration of antisense oligonucleotides significantly inhibited ischemia/reperfusion-induced TNF-α expression. Direct delivery into the left ventricular cavity was more effective than intravenous administration, and delivery just prior to ischemia was most effective in attenuating TNF-α expression. Furthermore, attenuation of TNF-α expression also significantly inhibited other post-ischemic inflammatory mediators including IL-1β and intercellular adhesion molecule-1 (ICAM-1). Thus, ultrasound-targeted antisense oligonucleotides can effectively attenuate post-ischemic cytokine expression when delivered in a clinically relevant time frame, obviating the need for pretreatment. [Copyright &y& Elsevier]

Published

2003

6. TRAF3IP2 mediates TWEAK/TWEAKR-induced pro-fibrotic responses in cultured cardiac fibroblasts and the heart.

Author

Das, Nitin A., Carpenter, Andrea J., Yoshida, Tadashi, Kumar, Senthil A., Gautam, Sandeep, Mostany, Ricardo, Izadpanah, Reza, Kumar, Ashok, Mummidi, Srinivas, Siebenlist, Ulrich, and Chandrasekar, Bysani

Subjects

*ADAPTOR proteins, *TUMOR necrosis factor receptors, *FIBROBLASTS, *CYTOKINE receptors, *VENTRICULAR remodeling, *THERAPEUTICS

Abstract

Persistent inflammation promotes development and progression of heart failure (HF). TWEAK (TNF-Related WEAK Inducer Of Apoptosis), a NF-κB- and/or AP-1-responsive proinflammatory cytokine that signals via TWEAK receptor (TWEAKR), is expressed at high levels in human and preclinical models of HF. Since the adapter molecule TRAF3IP2 (TRAF3 Interacting Protein 2) is an upstream regulator of various proinflammatory pathways, including those activated by NF-κB and AP-1, we hypothesized that targeting TRAF3IP2 inhibits TWEAK-induced proinflammatory and pro-fibrotic responses in vitro and in vivo. Consistent with the hypothesis, forced expression of TRAF3IP2 upregulated TWEAK and its receptor expression in cultured adult mouse cardiac fibroblasts (CF). Further, exogenous TWEAK upregulated TRAF3IP2 expression in a time- and dose-dependent manner, suggesting a positive-feedback regulation of TRAF3IP2 and TWEAK. TWEAK also promoted TRAF3IP2 nuclear translocation. Confirming its critical role in TWEAK signaling, silencing TRAF3IP2 inhibited TWEAK autoregulation, TWEAKR upregulation, p38 MAPK, NF-κB and AP-1 activation, inflammatory cytokine expression, MMP and TIMP1 activation, collagen expression and secretion, and importantly, proliferation and migration. Recapitulating these in vitro results, continuous infusion of TWEAK for 7 days increased systolic blood pressure (SBP), upregulated TRAF3IP2 expression, activated p38 MAPK, NF-κB and AP-1, induced the expression of multiple proinflammatory and pro-fibrotic mediators, and interstitial fibrosis in hearts of wild type mice. These proinflammatory and pro-fibrotic changes occurred in conjunction with myocardial hypertrophy and contractile dysfunction. Importantly, genetic ablation of TRAF3IP2 inhibited these TWEAK-induced adverse cardiac changes independent of increases in SBP, indicating that TRAF3IP2 plays a causal role, and thus a therapeutic target, in chronic inflammatory and fibro-proliferative diseases. [ABSTRACT FROM AUTHOR]

Published

2018

7. Metformin inhibits aldosterone-induced cardiac fibroblast activation, migration and proliferation in vitro, and reverses aldosterone + salt-induced cardiac fibrosis in vivo.

Author

Mummidi, Srinivas, Das, Nitin A., Carpenter, Andrea J., Kandikattu, Hemanthkumar, Krenz, Maike, Siebenlist, Ulrich, Valente, Anthony J., and Chandrasekar, Bysani

Subjects

*METFORMIN, *HEART diseases, *THERAPEUTICS, *HEART fibrosis, *CELL migration, *PHARMACOLOGY, *IN vitro studies

Abstract

The overall goals of this study were to investigate whether metformin exerts anti-fibrotic effects in aldosterone (Aldo) + salt-treated wild type mouse hearts, and determine the underlying molecular mechanisms in isolated adult cardiac fibroblasts (CF). In vitro, Aldo induced CF activation, migration, and proliferation, and these effects were inhibited by metformin. Further, Aldo induced PPM1A (Protein Phosphatase Magnesium Dependent 1A) activation and inhibited AMPK phosphorylation. At a pharmacologically relevant concentration, metformin restored AMPK activation, and inhibited Aldo-induced Nox4/H 2 O 2 -dependent TRAF3IP2 induction, pro-inflammatory cytokine expression, and CF migration and proliferation. Further, metformin potentiated the inhibitory effects of spironolactone, a mineralocorticoid receptor antagonist, on Aldo-induced collagen expression, and CF migration and proliferation. These results were recapitulated in vivo, where metformin reversed Aldo + salt-induced oxidative stress, suppression of AMPK activation, TRAF3IP2 induction, pro-inflammatory cytokine expression, and cardiac fibrosis, without significantly modulating systolic blood pressure. These in vitro and in vivo data indicate that metformin has the potential to reduce adverse cardiac remodeling in hypertensive heart disease. [ABSTRACT FROM AUTHOR]

Published

2016

8. Pressure overload induces IL-18 and IL-18R expression, but markedly suppresses IL-18BP expression in a rabbit model. IL-18 potentiates TNF-α-induced cardiomyocyte death.

Author

Yoshida, Tadashi, Friehs, Ingeborg, Mummidi, Srinivas, del Nido, Pedro J., Addulnour-Nakhoul, Solange, Delafontaine, Patrice, Valente, Anthony J., and Chandrasekar, Bysani

Subjects

*INTERLEUKINS, *GENE expression, *LABORATORY rabbits, *TUMOR necrosis factors, *HEART cells, *INFLAMMATION, *HYPERTROPHY, *PHYSIOLOGY

Abstract

Recurrent or sustained inflammation plays a causal role in the development and progression of left ventricular hypertrophy (LVH) and its transition to failure. Interleukin (IL)-18 is a potent pro-hypertrophic inflammatory cytokine. We report that induction of pressure overload in the rabbit, by constriction of the descending thoracic aorta induces compensatory hypertrophy at 4 weeks (mass/volume ratio: 1.7 ± 0.11) and ventricular dilatation indicative of heart failure at 6 weeks (mass/volume ratio: 0.7 ± 0.04). In concordance with this, fractional shortening was preserved at 4 weeks, but markedly attenuated at 6 weeks. We cloned rabbit IL-18, IL-18Rα, IL-18Rβ, and IL-18 binding protein (IL-18BP) cDNA, and show that pressure overload, while enhancing IL-18 and IL-18R expression in hypertrophied and failing hearts, markedly attenuated the level of expression of the endogenous IL-18 antagonist IL-18BP. Cyclical mechanical stretch (10% cyclic equibiaxial stretch, 1 Hz) induced hypertrophy of primary rabbit cardiomyocytes in vitro and enhanced ANP, IL-18, and IL-18Rα expression. Further, treatment with rhIL-18 induced its own expression and that of IL-18Rα via AP-1 activation, and induced cardiomyocyte hypertrophy in part via PI3K/Akt/GATA4 signaling. In contrast, IL-18 potentiated TNF-α-induced cardiomyocyte death, and by itself induced cardiac endothelial cell death. These results demonstrate that pressure overload is associated with enhanced IL-18 and its receptor expression in hypertrophied and failingrabbit hearts. Since IL-18BP expression is markedly inhibited, our results indicate a positive amplification in IL-18 proinflammatory signaling during pressure overload, and suggest IL-18 as a potential therapeutic target in pathological hypertrophy and cardiac failure. [ABSTRACT FROM AUTHOR]

Published

2014

9. Angiotensin II stimulates cardiac fibroblast migration via the differential regulation of matrixins and RECK.

Author

Siddesha, Jalahalli M., Valente, Anthony J., Sakamuri, Siva S.V.P., Yoshida, Tadashi, Gardner, Jason D., Somanna, Naveen, Takahashi, Chiaki, Noda, Makoto, and Chandrasekar, Bysani

Subjects

*ANGIOTENSIN II, *FIBROBLASTS, *HEART cells, *CELL motility, *EXTRACELLULAR matrix proteins, *GENETIC regulation, *CYSTEINE

Abstract

Abstract: Sustained induction and activation of matrixins (matrix metalloproteinases or MMPs), and the destruction and deposition of extracellular matrix (ECM), are the hallmarks of cardiac fibrosis. The reversion-inducing-cysteine-rich protein with Kazal motifs (RECK) is a unique membrane-anchored endogenous MMP regulator. We hypothesized that elevated angiotensin II (Ang II), which is associated with fibrosis in the heart, differentially regulates MMPs and RECK both in vivo and in vitro. Continuous infusion of Ang II into male C57Bl/6 mice for 2weeks resulted in cardiac fibrosis, with increased expressions of MMPs 2, 7, 9 and 14, and of collagens Ia1 and IIIa1. The expression of RECK, however, was markedly suppressed. These effects were inhibited by co-treatment with the Ang II type 1 receptor (AT1) antagonist losartan. In vitro, Ang II suppressed RECK expression in adult mouse cardiac fibroblasts (CF) via AT1/Nox4-dependent ERK/Sp1 activation, but induced MMPs 2, 14 and 9 via NF-κB, AP-1 and/or Sp1 activation. Further, while forced expression of RECK inhibits, its knockdown potentiates Ang II-induced CF migration. Notably, RECK overexpression reduced Ang II-induced MMPs 2, 9 and 14 activation, but enhanced collagens Ia1 and IIIa1 expression and soluble collagen release. These results demonstrate for the first time that Ang II suppresses RECK, but induces MMPs both in vivo and in vitro, and RECK overexpression blunts Ang II-induced MMP activation and CF migration in vitro. Strategies that upregulate RECK expression in vivo have the potential to attenuate sustained MMP expression, and blunt fibrosis and adverse remodeling in hypertensive heart diseases. [Copyright &y& Elsevier]

Published

2013

10. CIKS (Act1 or TRAF3IP2) mediates Angiotensin-II-induced Interleukin-18 expression, and Nox2-dependent cardiomyocyte hypertrophy

Author

Valente, Anthony J., Clark, Robert A., Siddesha, Jalahalli M., Siebenlist, Ulrich, and Chandrasekar, Bysani

Subjects

*ANGIOTENSIN II, *INTERLEUKIN-18, *GENE expression, *HEART cells, *CARDIAC hypertrophy, *INFLAMMATION, *HEART failure, *ATRIAL natriuretic peptides, *GREEN fluorescent protein

Abstract

Abstract: Chronic elevation of angiotensin (Ang)-II can lead to myocardial inflammation, hypertrophy and cardiac failure. The adaptor molecule CIKS (connection to IKK and SAPK/JNK) activates the IκB kinase/nuclear factor (NF)-κB and JNK/activator protein (AP)-1 pathways in autoimmune and inflammatory diseases. Since Ang-II is a potent activator of NF-κB and AP-1, we investigated whether CIKS is critical in Ang-II-mediated cardiac hypertrophy. Here we report that Ang-II induced CIKS mRNA and protein expression, CIKS binding to IKK and JNK perhaps functioning as a scaffold protein, CIKS-dependent IKK/NF-κB and JNK/AP-1 activation, p65 and c-Jun phosphorylation and nuclear translocation, NF-κB- and AP-1-dependent IL-18 and MMP-9 induction, and hypertrophy of adult cardiomyocytes isolated from WT, but not CIKS-null mice. These results were recapitulated in WT-cardiomyocytes following CIKS knockdown. Infusion of Ang-II for 7days induced cardiac hypertrophy, increased collagen content, and upregulated CIKS mRNA and protein expression in WT mice, whereas cardiac hypertrophy and collagen deposition were markedly attenuated in the CIKS-null mice, despite a similar increase in systolic blood pressure and DPI-inhibitable superoxide generation in both types of animals. Further, Ang-II-induced IKK/p65 and JNK/c-Jun phosphorylation, NF-κB and AP-1 activation, and IL-18 and MMP-9 expression were also markedly attenuated in CIKS-null mice. These results demonstrate that CIKS is critical in Ang-II-induced cardiomyocyte hypertrophy and fibrosis, and that CIKS is an important intermediate in Ang-II-induced redox signaling. CIKS is a potential therapeutic target in cardiac hypertrophy, fibrosis, and congestive heart failure. [Copyright &y& Elsevier]

Published

2012

11. β2 adrenergic activation induces the expression of IL-18 binding protein, a potent inhibitor of isoproterenol induced cardiomyocyte hypertrophy in vitro and myocardial hypertrophy in vivo

Author

Murray, David R., Mummidi, Srinivas, Valente, Anthony J., Yoshida, Tadashi, Somanna, Naveen K., Delafontaine, Patrice, Dinarello, Charles A., and Chandrasekar, Bysani

Subjects

*SYMPATHOMIMETIC agents, *GENE expression, *INTERLEUKIN-18, *HEART failure, *SYMPATHETIC nervous system, *HEART cells, *CARRIER proteins, *ISOPROTERENOL, *TRANSCRIPTION factors, *CARDIAC hypertrophy, *LABORATORY mice

Abstract

Abstract: Both the sympathetic nervous system and the proinflammatory cytokine interleukin-18 (IL-18) play key roles in the pathophysiology of the hypertrophied failing heart. IL-18 binding protein (IL-18BP), a natural inhibitor of IL-18, counters its biological effects. β-AR stimulation induces IL-18 expression, but whether it also regulates IL-18BP is not known. Here we demonstrate that the β-AR agonist isoproterenol (ISO) increases steady state IL-18BP mRNA and protein levels in adult mouse cardiomyocytes in a β2-AR-dependent manner. We cloned mouse Il18bp 5′cis-regulatory region, and identified putative CREB and C/EBPβ transcription factor-binding sites. Forced expression of mutant CREB or C/EBPβ knockdown markedly attenuated ISO-induced Il18bp transcription and deletion or mutation of CREB and C/EBP motifs in the Il18bp promoter reduced ISO-induced promoter-reporter gene activity. ISO induced CREB and C/EBPβ activation in cardiomyocytes via PI3K/Akt and ERK1/2. Importantly, ISO-induced hypertrophy in vitro was dependent on IL-18 induction as it was blunted by IL-18 neutralizing antibodies and forced expression of IL-18BP. Moreover, ISO-induced hypertrophy was markedly attenuated in IL-18 null and IL-18BP transgenic mice. These data support the novel concept that β-AR activation, in addition to inducing cardiomyocyte hypertrophy via IL-18, concomitantly induces a countering effect by stimulating IL-18BP expression, and that ISO-induced cardiomyocyte hypertrophy may result from a net effect of IL-18 and IL-18BP induction. [Copyright &y& Elsevier]

Published

2012

12. Angiotensin-II type 1 receptor and NOX2 mediate TCF/LEF and CREB dependent WISP1 induction and cardiomyocyte hypertrophy

Author

Shanmugam, Prakashsrinivasan, Valente, Anthony J., Prabhu, Sumanth D., Venkatesan, Balachandar, Yoshida, Tadashi, Delafontaine, Patrice, and Chandrasekar, Bysani

Subjects

*ANGIOTENSIN II, *MULTIENZYME complexes, *TRANSCRIPTION factors, *ENZYME activation, *ENZYME induction, *HEART cells, *CARDIAC hypertrophy, *GENE expression

Abstract

Abstract: Angiotensin-II (Ang-II) plays a key role in myocardial hypertrophy, remodeling and failure. We investigated whether Ang-II-induced cardiomyocyte hypertrophy is dependent on WNT1 inducible signaling pathway protein 1 (WISP1), a pro growth factor. Ang-II induced hypertrophy and WISP1 expression in neonatal rat cardiomyocytes (NRCM), effects that were significantly inhibited by pre-treatment with the AT1 antagonist losartan and by WISP1 knockdown. Further, Ang-II induced WISP1 was superoxide-dependent, and inhibited by DPI, an inhibitor of NADPH oxidases, and by knockdown of NOX2. AT1 was physically associated with NOX2 both in vitro and in vivo, and Ang-II increased this interaction in vivo. Ang-II induced WISP1 expression via superoxide/Akt/GSK3β/β-catenin/TCF/LEF and by Akt-dependent CREB activation. Further, Ang-II also activated CREB via superoxide-mediated p38 MAPK and ERK activation. Continuous infusion of Ang-II for 7days induced myocardial hypertrophy in rats, and was associated with increased Akt, p-Akt, p-p38 MAPK, p-ERK1/2, and WISP1 expression. These results demonstrate that Ang-II induced cardiomyocyte hypertrophy is mediated through AT1, NOX2 and the induction of WISP1, and may involve the direct interaction of AT1 with NOX2. Thus targeting both WISP1 and NOX2 may have a therapeutic potential in improving cardiomyocyte survival and growth following myocardial injury and remodeling. This article is part of a Special Issue entitled ‘Possible Editorial’. [Copyright &y& Elsevier]

Published

2011

13. EMMPRIN activates multiple transcription factors in cardiomyocytes, and induces interleukin-18 expression via Rac1-dependent PI3K/Akt/IKK/NF-κB andMKK7/JNK/AP-1 signaling

Author

Venkatesan, Balachandar, Valente, Anthony J., Prabhu, Sumanth D., Shanmugam, Prakashsrinivasan, Delafontaine, Patrice, and Chandrasekar, Bysani

Subjects

*INTERLEUKINS, *TRANSCRIPTION factors, *CARDIAC hypertrophy, *GENE expression, *HEART failure, *HEART cells, *EXTRACELLULAR matrix proteins, *METALLOPROTEINASES

Abstract

Abstract: The transmembrane glycoprotein extracellular matrix metalloproteinase inducer (EMMPRIN), and the pleiotropic proinflammatory cytokine interleukin (IL)-18, play critical roles in myocardial remodeling, by inducing matrix degrading metalloproteinases (MMPs). Previously we showed that IL-18 induces EMMPRIN expression in cardiomyocytes via MyD88/IRAK4/TRAF6/JNK-dependent Sp1 activation. Here in reciprocal studies we demonstrate that EMMPRIN is a potent inducer of IL-18 transcription, protein expression and protein secretion in primary mouse cardiomyocytes. We show for the first time that EMMPRIN stimulates the activation of NF-κB, AP-1, CREB, and ATF-2 in cardiomyocytes, and induces IL-18 expression via Rac1-dependent PI3K/Akt/IKK/NF-κB and MKK7/JNK/AP-1 signaling. Moreover, EMMPRIN induces robust time-dependent induction of various MMP mRNAs. EMMPRIN also induces the mRNA of TIMPs 1 and 3, but in a delayed fashion. These results suggest that IL-18-induced EMMPRIN expression may favor net MMP expression and ECM destruction, and thus identify both as potential therapeutic targets in countering adverse myocardial remodeling. [Copyright &y& Elsevier]

Published

2010

14. Interleukin-18 knockout mice display maladaptive cardiac hypertrophy in response to pressure overload

Author

Colston, James T., Boylston, William H., Feldman, Marc D., Jenkinson, Chris P., de la Rosa, Sam D., Barton, Amanda, Trevino, Rodolfo J., Freeman, Gregory L., and Chandrasekar, Bysani

Subjects

*INTERLEUKINS, *CARDIAC hypertrophy, *CYTOKINES, *GENE expression

Abstract

Abstract: Interleukin (IL)-18 is a cardiotropic proinflammatory cytokine chronically elevated in the serum of patients with cardiac hypertrophy (LVH). The purpose of this study was to examine the role of IL-18 in pressure-overload hypertrophy using wild type (WT) and IL-18 −/− (null) mice. Adult male C57Bl/6 mice underwent transaortic constriction (TAC) for 7days or sham surgery. Heart weight/body weight ratios showed blunted hypertrophy in IL-18 null TAC mice compared to WT TAC animals. Microarray analyses indicated differential expression of hypertrophy-related genes in WT versus IL-18 nulls. Northern, Western, and EMSA analyses showed Akt and GATA4 were increased in WT but unchanged in IL-18 null mice. Our results demonstrate blunted hypertrophy with reduced expression of contractile-, hypertrophy-, and remodeling-associated genes following pressure overload in IL-18 null mice, and suggest that IL-18 plays a critical role in the hypertrophic response. [Copyright &y& Elsevier]

Published

2007

15. TLR4-NOX4-AP-1 signaling mediates lipopolysaccharide-induced CXCR6 expression in human aortic smooth muscle cells

Author

Patel, Devang N., Bailey, Steven R., Gresham, John K., Schuchman, David B., Shelhamer, James H., Goldstein, Barry J., Foxwell, Brian M., Stemerman, Michael B., Maranchie, Jodi K., Valente, Anthony J., Mummidi, Srinivas, and Chandrasekar, Bysani

Subjects

*CHEMOKINES, *ENDOTOXINS, *MESSENGER RNA, *CYTOKINES

Abstract

Abstract: CXCL16 is a transmembrane non-ELR CXC chemokine that signals via CXCR6 to induce aortic smooth muscle cell (ASMC) proliferation. While bacterial lipopolysaccharide (LPS) has been shown to stimulate CXCL16 expression in SMC, its effects on CXCR6 are not known. Here, we demonstrate that LPS upregulates CXCR6 mRNA, protein, and surface expression in human ASMC. Inhibition of TLR4 with neutralizing antibodies or specific siRNA interference blocked LPS-mediated CXCR6 expression. LPS stimulated both AP-1 (c-Fos, c-Jun) and NF-κB (p50 and p65) activation, but only inhibition of AP-1 attenuated LPS-induced CXCR6 expression. Using dominant negative expression vectors and siRNA interference, we demonstrate that LPS induces AP-1 activation via MyD88, TRAF6, ERK1/2, and JNK signaling pathways. Furthermore, the flavoprotein inhibitor diphenyleniodonium chloride significantly attenuated LPS-mediated AP-1-dependent CXCR6 expression, as did inhibition of NOX4 NADPH oxidase by siRNA. Finally, CXCR6 knockdown inhibited CXCL16-induced ASMC proliferation. These results demonstrate that LPS-TLR4-NOX4-AP-1 signaling can induce CXCR6 expression in ASMC, and suggest that the CXCL16–CXCR6 axis may be an important proinflammatory pathway in the pathogenesis of atherosclerosis. [Copyright &y& Elsevier]

Published

2006

16. β-Adrenergic receptor blockade modulates Bcl-XS expression and reduces apoptosis in failing myocardium

Author

Prabhu, Sumanth D., Wang, Guangwu, Luo, Jianzhu, Gu, Yan, Ping, Peipei, and Chandrasekar, Bysani

Subjects

*ADRENERGIC receptors, *APOPTOSIS

Abstract

The mechanisms by which β-adrenergic receptor (β-AR) blockade modulates apoptosis in heart failure (HF) are unclear. We examined the impact of β-AR blockade with metoprolol on myocardial remodeling, apoptosis, pro-apoptotic (Fas, Fas ligand, Bax, and Bcl-XS) and anti-apoptotic (Bcl-XLand Bcl-2) gene expression, and Bcl-XL and Bcl-XS protein in post-infarction HF in rats. In untreated rats, there was significant (P < 0.001) LV dilatation and systolic dysfunction compared to sham. Myocardial apoptosis was significantly increased (P < 0.005). Fas, Bax, and Bcl-2 mRNA expression was unchanged. However, Fas ligand mRNA and Bcl-XS mRNA and protein, all undetectable in sham, were markedly elevated (P < 0.001), whereas Bcl-XL mRNA and protein was unchanged. Immunohistochemistry confirmed increased Bcl-XS staining in failing myocardium, with unchanged Bcl-XL. Metoprolol treatment resulted in: (1) improved LV remodeling (P < 0.025), (2) reduced myocardial apoptosis (P < 0.005), and (3) selective reduction in myocardial Bcl-XS expression (P < 0.001) without change in Fas, Fas ligand, Bax, Bcl-2, or Bcl-XL. Studies in isolated rat myocytes revealed that prolonged isoproterenol (ISO) stimulation significantly increased Bcl-XS protein, reducing the Bcl-XL/XS ratio and myocyte survival (P < 0.005). ISO-induced Bcl-XS expression was significantly attenuated (P < 0.001) by both metoprolol and CGP20712A, a β1-AR selective antagonist, but not by ICI118,551, a β2-AR selective antagonist. We conclude that adrenergic activation, such as occurs in HF, increases pro-apoptotic Bcl-XS expression via the β1-AR. β-AR blockade in HF reduces myocardial apoptosis; attenuation of Bcl-XS expression may be one mechanism underlying this effect. [Copyright &y& Elsevier]

Published

2003