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Start Over Author "Brown, Joan Heller" Journal journal of biological chemistry
45 results on '"Brown, Joan Heller"'

1. Reductions in the Cardiac Transient Outward K+ Current I to Caused by Chronic β-Adrenergic Receptor Stimulation Are Partly Rescued by Inhibition of Nuclear Factor κB*

Author

Panama, Brian K, Korogyi, Adam S, Aschar-Sobbi, Roozbeh, Oh, Yena, Gray, Charles BB, Gang, Hongying, Brown, Joan Heller, Kirshenbaum, Lorrie A, and Backx, Peter H

Subjects
Genetics, Cardiovascular, Heart Disease, Prevention, 2.1 Biological and endogenous factors, Aetiology, Adrenergic beta-Agonists, Animals, Calcineurin, Calcium-Calmodulin-Dependent Protein Kinase Type 2, Gene Expression Regulation, Isoproterenol, Kv Channel-Interacting Proteins, Myocytes, Cardiac, NF-kappa B, Rats, Rats, Sprague-Dawley, Receptors, Adrenergic, Shal Potassium Channels, Transcription, Genetic, adrenergic receptor, Ca2+, calmodulin-dependent protein kinase, cardiomyocyte, potassium channel, transcription, Ca2+/calmodulin-dependent protein kinase, Chemical Sciences, Biological Sciences, Medical and Health Sciences, Biochemistry & Molecular Biology
Abstract

The fast transient outward potassium current (Ito,f) plays a critical role in the electrical and contractile properties of the myocardium. Ito,f channels are formed by the co-assembly of the pore-forming α-subunits, Kv4.2 and Kv4.3, together with the accessory β-subunit KChIP2. Reductions of Ito,f are common in the diseased heart, which is also associated with enhanced stimulation of β-adrenergic receptors (β-ARs). We used cultured neonatal rat ventricular myocytes to examine how chronic β-AR stimulation decreases Ito,f. To determine which downstream pathways mediate these Ito,f changes, adenoviral infections were used to inhibit CaMKIIδc, CaMKIIδb, calcineurin, or nuclear factor κB (NF-κB). We observed that chronic β-AR stimulation with isoproterenol (ISO) for 48 h reduced Ito,f along with mRNA expression of all three of its subunits (Kv4.2, Kv4.3, and KChIP2). Inhibiting either CaMKIIδc nor CaMKIIδb did not prevent the ISO-mediated Ito,f reductions, even though CaMKIIδc and CaMKIIδb clearly regulated Ito,f and the mRNA expression of its subunits. Likewise, calcineurin inhibition did not prevent the Ito,f reductions induced by β-AR stimulation despite strongly modulating Ito,f and subunit mRNA expression. In contrast, NF-κB inhibition partly rescued the ISO-mediated Ito,f reductions in association with restoration of KChIP2 mRNA expression. Consistent with these observations, KChIP2 promoter activity was reduced by p65 as well as β-AR stimulation. In conclusion, NF-κB, and not CaMKIIδ or calcineurin, partly mediates the Ito,f reductions induced by chronic β-AR stimulation. Both mRNA and KChIP2 promoter data suggest that the ISO-induced Ito,f reductions are, in part, mediated through reduced KChIP2 transcription caused by NF-κB activation.

Published
2016

2. Thrombin Promotes Sustained Signaling and Inflammatory Gene Expression through the CDC25 and Ras-associating Domains of Phospholipase Cϵ*

Author

Dusaban, Stephanie S, Kunkel, Maya T, Smrcka, Alan V, and Brown, Joan Heller

Subjects
Genetics, Animals, Animals, Newborn, Astrocytes, Cell Compartmentation, Fluorescence Resonance Energy Transfer, Gene Expression Regulation, Golgi Apparatus, Inflammation, Inositol 1, 4, 5-Trisphosphate, Mice, Mice, Inbred C57BL, Mice, Transgenic, Phosphoinositide Phospholipase C, Primary Cell Culture, Protein Kinase C, Protein Structure, Tertiary, Signal Transduction, Thrombin, rap1 GTP-Binding Proteins, ras-GRF1, G protein-coupled receptor, Phospholipase C, Ras-related protein 1, astrocyte, cyclooxygenase, diacylglycerol, guanine nucleotide exchange factor, protein kinase D, thrombin, Chemical Sciences, Biological Sciences, Medical and Health Sciences, Biochemistry & Molecular Biology
Abstract

Phospholipase C-epsilon (PLCϵ) plays a critical role in G-protein-coupled receptor-mediated inflammation. In addition to its ability to generate the second messengers inositol 1,4,5-trisphosphate and diacylglycerol, PLCϵ, unlike the other phospholipase C family members, is activated in a sustained manner. We hypothesized that the ability of PLCϵ to function as a guanine nucleotide exchange factor (GEF) for Rap1 supports sustained downstream signaling via feedback of Rap1 to the enzyme Ras-associating (RA2) domain. Using gene deletion and adenoviral rescue, we demonstrate that both the GEF (CDC25 homology domain) and RA2 domains of PLCϵ are required for long term protein kinase D (PKD) activation and subsequent induction of inflammatory genes. PLCϵ localization is largely intracellular and its compartmentalization could contribute to its sustained activation. Here we show that localization of PLCϵ to the Golgi is required for activation of PKD in this compartment as well as for subsequent induction of inflammatory genes. These data provide a molecular mechanism by which PLCϵ mediates sustained signaling and by which astrocytes mediate pathophysiological inflammatory responses.

Published
2015

3. The Ras-related Protein, Rap1A, Mediates Thrombin-stimulated, Integrin-dependent Glioblastoma Cell Proliferation and Tumor Growth*

Author

Sayyah, Jacqueline, Bartakova, Alena, Nogal, Nekeisha, Quilliam, Lawrence A, Stupack, Dwayne G, and Brown, Joan Heller

Subjects
Biotechnology, Cancer, Rare Diseases, Brain Disorders, Brain Cancer, Aetiology, 2.1 Biological and endogenous factors, Animals, Cell Line, Tumor, Cell Proliferation, Gene Expression Regulation, Neoplastic, Glioblastoma, Heterografts, Humans, Integrin beta1, Mice, Neoplasm Proteins, Neoplasm Transplantation, Thrombin, rap1 GTP-Binding Proteins, rhoA GTP-Binding Protein, Cell Signaling, G-protein-coupled Receptor, Integrin, Rap1, Small GTPase, Chemical Sciences, Biological Sciences, Medical and Health Sciences, Biochemistry & Molecular Biology
Abstract

Rap1 is a Ras family GTPase with a well documented role in ERK/MAP kinase signaling and integrin activation. Stimulation of the G-protein-coupled receptor PAR-1 with thrombin in human 1321N1 glioblastoma cells led to a robust increase in Rap1 activation. This response was sustained for up to 6 h and mediated through RhoA and phospholipase D (PLD). Thrombin treatment also induced a 5-fold increase in cell adhesion to fibronectin, which was blocked by down-regulating PLD or Rap1A or by treatment with a β1 integrin neutralizing antibody. In addition, thrombin treatment led to increases in phospho-focal adhesion kinase (tyrosine 397), ERK1/2 phosphorylation and cell proliferation, which were significantly inhibited in cells treated with β1 integrin antibody or Rap1A siRNA. To assess the role of Rap1A in tumor formation in vivo, we compared growth of 1321N1 cells stably expressing control, Rap1A or Rap1B shRNA in a mouse xenograft model. Deletion of Rap1A, but not of Rap1B, reduced tumor mass by >70% relative to control. Similar observations were made with U373MG glioblastoma cells in which Rap1A was down-regulated. Collectively, these findings implicate a Rap1A/β1 integrin pathway, activated downstream of G-protein-coupled receptor stimulation and RhoA, in glioblastoma cell proliferation. Moreover, our data demonstrate a critical role for Rap1A in glioblastoma tumor growth in vivo.

Published
2014

8. CaMKIIδ Isoforms Differentially Affect Calcium Handling but Similarly Regulate HDAC/MEF2 Transcriptional Responses

Author

Zhang, Tong, primary, Kohlhaas, Michael, additional, Backs, Johannes, additional, Mishra, Shikha, additional, Phillips, William, additional, Dybkova, Nataliya, additional, Chang, Shurong, additional, Ling, Haiyun, additional, Bers, Donald M., additional, Maier, Lars S., additional, Olson, Eric N., additional, and Brown, Joan Heller, additional

Published
2007
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16. The Cardiac-specific Nuclear δB Isoform of Ca2+/Calmodulin-dependent Protein Kinase II Induces Hypertrophy and Dilated Cardiomyopathy Associated with Increased Protein Phosphatase 2A Activity

Author

Zhang, Tong, primary, Johnson, Eric N., additional, Gu, Yusu, additional, Morissette, Michael R., additional, Sah, Valerie P., additional, Gigena, Marisa S., additional, Belke, Darrell D., additional, Dillmann, Wolfgang H., additional, Rogers, Terry B., additional, Schulman, Howard, additional, Ross, John, additional, and Brown, Joan Heller, additional

Published
2002
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32. The cardiac-specific nuclear delta(B) isoform of Ca2+/calmodulin-dependent protein kinase II induces hypertrophy and dilated cardiomyopathy associated with increased protein phosphatase 2A activity.

Author

Zhang, Tong, Johnson, Eric N, Gu, Yusu, Morissette, Michael R, Sah, Valerie P, Gigena, Marisa S, Belke, Darrell D, Dillmann, Wolfgang H, Rogers, Terry B, Schulman, Howard, Ross, John, and Brown, Joan Heller

Abstract

The delta isoform of Ca(2+)/calmodulin-dependent protein kinase II (CaMKII) predominates in the heart. To investigate the role of CaMKII in cardiac function, we made transgenic (TG) mice that express the nuclear delta(B) isoform of CaMKII. The expressed CaMKIIdelta(B) transgene was restricted to the myocardium and highly concentrated in the nucleus. Cardiac hypertrophy was evidenced by an increased left ventricle to body weight ratio and up-regulation of embryonic and contractile protein genes including atrial natriuretic factor, beta-myosin heavy chain, and alpha-skeletal actin. Echocardiography revealed ventricular dilation and decreased cardiac function, which was also observed in hemodynamic measurements from CaMKIIdelta(B) TG mice. Surprisingly, phosphorylation of phospholamban at both Thr(17) and Ser(16) was significantly decreased in the basal state as well as upon adrenergic stimulation. This was associated with diminished sarcoplasmic reticulum Ca(2+) uptake in vitro and altered relaxation properties in vivo. The activity and expression of protein phosphatase 2A were both found to be increased in CaMKII TG mice, and immunoprecipitation studies indicated that protein phosphatase 2A directly associates with CaMKII. Our findings are the first to demonstrate that CaMKII can induce hypertrophy and dilation in vivo and indicate that compensatory increases in phosphatase activity contribute to the resultant phenotype.

Published
2002
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33. Physical and Functional Interactions of Gαqwith Rho and Its Exchange Factors*

Author

Sagi, Sarah A., Seasholtz, Tammy M., Kobiashvili, Mariya, Wilson, Brenda A., Toksoz, Deniz, and Brown, Joan Heller

Abstract

Recent reports have shown that several heterotrimeric protein-coupled receptors that signal through Gαqcan induce Rho-dependent responses, but the pathways that mediate the interaction between Gαqand Rho have not yet been identified. In this report we present evidence that Gαqexpressed in COS-7 cells coprecipitates with the Rho guanine nucleotide exchange factor (GEF) Lbc. Furthermore, Gαqexpression enhances Rho-dependent responses. Coexpressed Gαqand Lbc have a synergistic effect on the Rho-dependent rounding of 1321N1 astrocytoma cells. In addition, serum response factor-dependent gene expression, as assessed by the SRE.L reporter gene, is synergistically activated by Gαqand Rho GEFs. The synergistic effect of Gαqon this response is inhibited by C3 exoenzyme and requires phospholipase C activation. Surprisingly, expression of Gαq, in contrast to that of Gα12and Gα13, does not increase the amount of activated Rho. We also observe that Gαqenhances SRE.L stimulation by activated Rho, indicating that the effect of Gαqoccurs downstream of Rho activation. Thus, Gαqinteracts physically and/or functionally with Rho GEFs; however this does not appear to lead to or result from increased activation of Rho. We suggest that Gαq-generated signals enhance responses downstream of Rho activation.

Published
2001
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34. Rho Is Required for Gαqand α1-Adrenergic Receptor Signaling in Cardiomyocytes

Author

Sah, Valerie P., Hoshijima, Masahiko, Chien, Kenneth R., and Brown, Joan Heller

Abstract

G protein-coupled receptor agonists initiate a cascade of signaling events in neonatal rat ventricular myocytes that culminates in changes in gene expression and cell growth characteristic of hypertrophy. These responses have been previously shown to be dependent on Gqand Ras. Rho, a member of the Ras superfamily of GTPases, regulates cytoskeletal rearrangement and transcriptional activation of the c-fosserum response element. Immunofluorescence staining of cardiomyocytes shows that Rho is present and predominantly cytosolic. We used two inhibitors of Rho function, dominant negative N19RhoA and Clostridium botulinumC3 transferase, to examine the possible requirement for Rho in α1-adrenergic receptor-mediated hypertrophy. Both inhibitors markedly attenuated atrial natriuretic factor (ANF) reporter gene expression induced by α1-adrenergic receptor stimulation with phenylephrine, and virtually abolished the increase in ANF reporter gene expression induced by GTPase-deficient Gαq. These effects were reproduced with the myosin light chain-2 reporter gene. Notably, N19RhoA did not block the ability of activated Ras to induce ANF and myosin light chain-2 reporter gene expression. Furthermore, activation of the extracellular signal-regulated kinase by phenylephrine was not blocked by N19RhoA, nor was it stimulated by an activated mutant of RhoA. Since activated RhoA and Ras produce a large synergistic effect on ANF-luciferase gene expression, we conclude that Rho functions in a pathway separate from but complementary to Ras. Our results provide direct evidence that Rho is an effector of Gαqsignaling and suggest for the first time that a low molecular weight GTPase other than Ras is involved in regulating myocardial cell growth and gene expression in response to heterotrimeric G protein-linked receptor activation.

Published
1996
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35. Gα12Stimulates c-Jun NH2-terminal Kinase through the Small G Proteins Ras and Rac*

Author

Collins, Lila R., Minden, Audrey, Karin, Michael, and Brown, Joan Heller

Abstract

The pertussis toxin (PTX) insensitive heterotrimeric G protein G12has been implicated in mitogenesis and transformation, but its direct effectors remain unknown. To define potential signaling pathways utilized by G12, we expressed an activated mutant of its α subunit, Gα12(Q229L), in HEK293 cells and examined its effects on Ras and mitogen-activated protein kinases (MAPKs). Transient expression of activated Gα12increased the percentage of Ras in the active, GTP-bound state, stimulated c-Jun NH2-terminal kinase (JNK) activity, and enhanced the transcriptional activity of c-Jun. Dominant negative Ras (N17Ras) inhibited Gα12-mediated JNK activation in NIH3T3 cells but failed to do so in HEK293 cells. In contrast, dominant negative Rac (N17Rac1) inhibited JNK activation by Gα12in HEK293 cells as well as three other cell lines. In 1321N1 cells, where thrombin stimulates G12-dependent mitogenesis, coexpression of N17Rac1 or a dominant negative mutant of MEKK1 (MEKKΔ(K432M)) inhibits c-Jun/AP-1 sensitive reporter gene expression stimulated by thrombin or Gα12. These data demonstrate that the α subunit of the heterotrimeric G protein G12, like tyrosine kinase growth factor receptors, activates Ras and recruits a signal transduction pathway involving the small GTP-binding protein Rac that leads to JNK activation.

Published
1996
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36. The Nuclear δBIsoform of Ca2+/Calmodulin-dependent Protein Kinase II Regulates Atrial Natriuretic Factor Gene Expression in Ventricular Myocytes*

Author

Ramirez, M. Teresa, Zhao, Xiao-Lan, Schulman, Howard, and Brown, Joan Heller

Abstract

Cultured neonatal ventricular myocytes display features of myocardial hypertrophy including increased cell size, myofilament organization, and reexpression of the embryonic gene for atrial natriuretic factor (ANF). KN-93, an inhibitor of multifunctional Ca2+/calmodulin-dependent protein kinase (CaM kinase II), blocked the induction of these responses by the α1-adrenergic receptor agonist phenylephrine, whereas its inactive analog KN-92 did not. To directly determine whether CaM kinase II could regulate ANF gene expression, we transiently expressed each of three isoforms of CaM kinase II (α, δB, and δC) along with an ANF promoter/luciferase reporter gene. The δBisoform markedly increased luciferase gene expression, whereas comparable levels of the δCand α isoforms were ineffective. Expression of δB-CaM kinase II also potentiated phenylephrine-mediated ANF gene expression, and this effect was blocked by KN-93 but not by KN-92. The ability of δB-CaM kinase II to transactivate a truncated ANF promoter, containing a serum response element (SRE) required for phenylephrine-inducible gene expression, was lost when this SRE was mutated. The δBisoform of CaM kinase II has been shown to exhibit nuclear localization. Coexpression of the non-nuclear δCor α isoforms, which can form multimers with the δBisoform, prevented the nuclear localization of δB-CaM kinase II and also blocked its effects on ANF reporter gene and protein expression. In addition, a chimeric α-CaM kinase II which contains the nuclear localization signal of the δBisoform was able to induce ANF reporter gene expression, albeit to a lesser extent than δB-CaM kinase II. These data are the first to assign a function to the δBisoform of CaM kinase II and to link its nuclear localization to subsequent activation of cardiac gene expression.

Published
1997
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37. G12Requirement for Thrombin-stimulated Gene Expression and DNA Synthesis in 1321N1 Astrocytoma Cells (∗)

Author

Aragay, Anna M., Collins, Lila R., Post, Ginell R., Watson, A. John, Feramisco, James R., Brown, Joan Heller, and Simon, Melvin I.

Abstract

Thrombin stimulation of 1321N1 astrocytoma cells leads to Ras-dependent AP-1-mediated transcriptional activation and to DNA replication. In contrast to what has been observed in most cell systems, in 1321N1 cells these responses are pertussis toxin-insensitive. The pertussis toxin-insensitive G-protein G12has been implicated in cell growth and transformation in different cell systems. We have examined the potential role of this protein in AP-1-mediated transcriptional activation and DNA synthesis in 1321N1 cells. Transient expression of an activated (GTPase-deficient) mutant of Gα12increased AP-1-dependent gene expression. This response was inhibited by co-expression of a dominant negative Ala-15 Ras protein. To determine whether the pertussis toxin-insensitive G12protein is involved in the thrombin-stimulated DNA synthesis, an inhibitory antibody against the C-terminal sequence of Gα12subunit was microinjected into 1321N1 cells. Microinjection of the anti-Gα12resulted in a concentration-dependent inhibition of thrombin-stimulated DNA synthesis. In contrast, microinjection of nonimmune IgG or an antibody directed against the C terminus of Gαodid not reduce the mitogenic response to thrombin. Furthermore, microinjection of the anti-Gα12antibody had no effect on fibroblast growth factor-stimulated DNA synthesis. These results demonstrate a specific role for Gα12in the mitogenic response to thrombin in human astroglial cells.

Published
1995
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38. The MEKK-JNK Pathway Is Stimulated by α1-Adrenergic Receptor and Ras Activation and Is Associated with in Vitroand in VivoCardiac Hypertrophy*

Author

Ramirez, M. Teresa, Sah, Valerie P., Zhao, Xiao-Lan, Hunter, John J., Chien, Kenneth R., and Brown, Joan Heller

Abstract

In neonatal rat ventricular myocytes, stimulation of the α1-adrenergic receptor (α1-AdrR) activates a program of genetic and morphological changes characterized by transcriptional activation of the atrial natriuretic factor (ANF) gene and enlargement (hypertrophy) of the cells. The low molecular weight GTPase Ras has been established as an important regulator of hypertrophy bothin vitroand in vivo. Ras activates a kinase cascade involving Raf, the mitogen-activated protein kinase kinase (MEK), and the extracellular signal-regulated protein kinase (ERK). However, the extent of involvement of this pathway in regulating hypertrophic responses is controversial. We demonstrate here that both α1-AdrR stimulation and Ras can also activate the c-Jun NH2-terminal kinase (JNK) in cardiomyocytes. The α1-AdrR effect on JNK occurs through a pathway requiring Ras and MEK kinase (MEKK). A constitutively activated mutant of MEKK that preferentially activates JNK, stimulates ANF reporter gene expression, while a dominant negative MEKK mutant inhibits ANF expression induced by PE. Furthermore, JNK activity is increased in the ventricles of mice overexpressing oncogenic Ras, whereas ERK activity is not. These results suggest that the α1-AdrR mediates ANF gene expression through a Ras-MEKK-JNK pathway and that activation of this pathway is associated with in vitroand in vivohypertrophy.

Published
1997
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39. Reductions in the Cardiac Transient Outward K+ Current /to Caused by Chronic β-Adrenergic Receptor Stimulation Are Partly Rescued by Inhibition of Nuclear Factor κB*.

Author

Panama, Brian K., Korogyi, Adam S., Aschar-Sobbi, Roozbeh, Yena Oh, Gray, Charles B. B., Hongying Gang, Brown, Joan Heller, Kirshenbaum, Lorrie A., and Backx, Peter H.

Subjects
*ADRENERGIC receptors, *POTASSIUM, *MYOCARDIUM, *ISOPROTERENOL, *NF-kappa B, *SYMPATHETIC nervous system
Abstract

The fast transient outward potassium current (Ito,f) plays a critical role in the electrical and contractile properties of the myocardium. Ito,f channels are formed by the co-assembly of the pore-forming α-subunits, Kv4.2 and Kv4.3, together with the accessoryβ-subunit KChIP2. Reductions of Ito,f arecommon in the diseased heart, which is also associated with enhanced stimulation of β-adrenergic receptors (β-ARs). We used cultured neonatal rat ventricular myocytes to examine how chronic β-AR stimulation decreases Ito,f. To determine which downstream pathways mediate these Ito,f changes, adenoviral infections were used to inhibit CaMKIIδc, CaMKIIδb, calcineurin, or nuclear factorκB (NF-κB).Weobserved that chronicβ-AR stimulation with isoproterenol (ISO) for 48 h reduced Ito,f along with mRNA expression of all three of its subunits (Kv4.2, Kv4.3, and KChIP2). Inhibiting either CaMKIIδc nor CaMKIIδb did not prevent the ISO-mediated Ito,f reductions, even though CaMKIIδc and CaMKIIδb clearly regulated Ito,f and the mRNA expression of its subunits. Likewise, calcineurin inhibition did not prevent the Ito,f reductions induced by β-AR stimulation despite strongly modulating Ito,f and subunit mRNA expression. In contrast, NF-κB inhibition partly rescued the ISO-mediated Ito,f reductions in association with restoration of KChIP2 mRNA expression. Consistent with these observations, KChIP2 promoter activity was reduced by p65 as well as β-AR stimulation. In conclusion, NF-κB, and not CaMKIIδ or calcineurin, partly mediates the Ito,f reductions induced by chronic β-AR stimulation. Both mRNA and KChIP2 promoter data suggest that the ISO-induced Ito,f reductions are, in part, mediated through reduced KChIP2 transcription caused by NF-κB activation. [ABSTRACT FROM AUTHOR]

Published
2016
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40. Akt Increases Sarcoplasmic Reticulum Ca2+ Cycling by Direct Phosphorylation of Phospholamban at Thr17.

Author

Catalucci, Daniele, Latronico, Michael V. G., Ceci, Marcello, Rusconi, Francesca, Young, Howard S., Gallo, Paolo, Santonastasi, Marco, Bellacosa, Alfonso, Brown, Joan Heller, and Condorelli, Gianluigi

Subjects
*HEART cells, *CELL physiology, *PHYSIOLOGICAL adaptation, *SARCOPLASMIC reticulum, *BIOLOGICAL assay, *PHOSPHORYLATION, *HYPERTROPHY, *LABORATORY mice
Abstract

Cardiomyocytes adapt to physical stress by increasing their size while maintaining cell function. The serine/threonine kinase Akt plays a critical role in this process of adaptation. We previously reported that transgenic overexpression of an active form of Akt (Akt-E4AI)K) in mice results in increased cardiac contractility and cell size, as well as improved sarcoplasmic reticulum (SR) Ca2+ handling. Because it is not fully elucidated, we decided to study the molecular mechanism by which Akt-E40K overexpression improves SR Ca2+ handling. To this end, SR Ca2+ uptake and the phosphorylation status of phospholamban (PLN) were evaluated in heart extracts from wild-type and Akt-E40K mice and mice harboring inducible and cardiac specffic knock-out of phosphatidylinositol-dependent kinase-1, the upstream activator of Akt. Moreover, the effect of Akt was assessed in vitro by overexpressing a mutant Akt targeted preferentially to the SR, and by biochemical assays to evaluate potential interaction with PLN. We found that when activated, Akt interacts with and phosphorylates PLN at Thr17, the Ca2+-calmodulin-dependent kinase IIδ site, whereas silencing Akt signaling, through the knock-out of phosphatidylinositol-dependent kinase-1, resulted in reduced phosphorylation of PLN at Thr17. Furthermore, overexpression of SR-targeted Akt in cardiomyocytes improved Ca2+ handling without affecting cell size. Thus, we describe here a new mechanism whereby the preferential translocation of Akt to the SR is responsible for enhancement of contractility without stimulation of hypertrophy. [ABSTRACT FROM AUTHOR]

Published
2009
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41. Si P1 Receptor Localization Confers Selectivity for Gi-mediated cAMP and Contractile Responses.

Author

Means, Christopher Kable, Miyamoto, Shigeki, Chun, Jerold, and Brown, Joan Heller

Subjects
*MUSCLE cells, *WHOOPING cough, *TOXINS, *ADENYLATE cyclase, *CELL receptors
Abstract

Adult mouse ventricular myocytes express S1P1, S1P2, and S1P3 receptors. S1P activates Akt and ERK in adult mouse ventricular myocytes through a pertussis toxin-sensitive (Gi/o-mediated) pathway. Akt and ERK activation by S1P are reduced ~30% in S1P3 and 60% in S1P2 receptor knock-out myocytes. With combined S1P2,3 receptor deletion, activation of Akt is abolished and ERK activation is reduced by nearly 90%. Thus the S1P1 receptor, while present in S1P23 receptor knock-out myocytes, is unable to mediate Akt or ERK activation. In contrast, S1P induces pertussis toxin-sensitive inhibition of isoproterenol-stimulated cAMP accumulation in both WT and S1P2,3 receptor knock-out myocytes demonstrating that the S1P1 receptor can functionally couple to Gi. An S1P1 receptor selective agonist, SEW2871, also decreased cAMP accumulation but failed to activate ERK or Akt. To determine whether localization of the S1P1 receptor mediates this signaling specificity, methyl-β-cyclodextrin (MβCD) treatment was used to disrupt caveolae. The S1P1 receptor was concentrated in caveolar fractions, and associated with caveolin-3 and this localization was disrupted by MβCD. S1P-mediated activation of ERK or Akt was not diminished but inhibition of cAMP accumulation by S1P and SEW2871 was abolished by MβCD treatment. S1P inhibits the positive inotropic response to isoproterenol and this response is also mediated through the S1P1 receptor and lost following caveolar disruption. Thus localization of S1P1 receptors to caveolae is required for the ability of this receptor to inhibit adenylyl cyclase and contractility but compromises receptor coupling to Akt and ERK. [ABSTRACT FROM AUTHOR]

Published
2008
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42. CaMKIIδ Isoforms Differentially Affect Calcium Handling but Similarly Regulate HDAC/MEF2 Transcriptional Responses.

Author

Tong Zhang, Kohlhaas, Michael, Backs, Johannes, Mishra, Shikha, Phillips, William, Dybkova, Nataliya, Shurong Chang, Haiyun Ling, Bers, Donald M., Maier, Lars S., OIson, Eric N., and Brown, Joan Heller

Subjects
*PHOSPHORYLATION, *SARCOPLASMIC reticulum, *PROTEIN kinases, *HEART cells, *RYANODINE
Abstract

The δB and δC splice variants of Ca2+/calmodulin-dependent protein kinase II (CaMKII), which differ by the presence of a nuclear localization sequence, are both expressed in cardiomyocytes. We used transgenic (TG) mice and CaMKII expression in cardiomyocytes to test the hypothesis that the CaMKIIδ isoform regulates cytosolic Ca2+ handling and the δB isoform, which localizes to the nucleus, regulates gene transcription. Phosphorylation of CaMKII sites on the ryanodine receptor (RyR) and on phospholamban (PLB) were increased in CaMKIIδC TG, This was associated with markedly enhanced sarcoplasmic reticulum (SR) Ca2+ spark frequency and decreased SR Ca2+ content in cardiomyocytes. None of these parameters were altered in TG mice expressing the nuclear-targeted CaMKIIδB. In contrast, cardiac expression of either CaMKIIδB or δC induced transactivation of myocyte enhancer factor 2 (MEF2) gene expression and up-regulated hypertrophic marker genes. Studies using rat ventricular cardiomyocytes con- firmed that CaMKIIδB and δC both regulate MEF2-luciferase gene expression, increase histone deacetylase 4 (HDAC4) association with 14-3-3, and induce HDAC4 translocation from nucleus to cytoplasm, indicating that either isoform can stimulate HDAC4 phosphorylation. Finally, HDAC4 kinase activity was shown to be increased in cardiac homogenates from either CaMKIIδB or δC TG mice. Thus CaMKIIδ isoforms have similar effects on hypertrophic gene expression but disparate effects on Ca2+ handling, suggesting distinct roles for CaMKIIδ isoform activation in the pathogenesis of cardiac hypertrophy versus heart failure. [ABSTRACT FROM AUTHOR]

Published
2007
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43. Ca2+ Dysregulation Induces Mitochondrial Depolarization and Apoptosis.

Author

Miyamoto, Shigeki, Howes, Amy L., Adams, John W., Dorn II, Gerald W., and Brown, Joan Heller

Subjects
*GENE expression, *HEART cells, *APOPTOSIS, *CELL membranes, *MITOCHONDRIA, *SARCOPLASMIC reticulum, *MESSENGER RNA, *GENETIC regulation, *HEART cytology
Abstract

We previously reported that constitutively activated Gαq (Q209L) expression in cardiomyocytes induces apoptosis through opening of the mitochondrial permeability transition pore. We assessed the hypothesis that disturbances in Ca2+ handling linked Gαq activity to apoptosis because resting Ca2+ levels were significantly increased prior to development of apoptosis. Treating cells with EGTA lowered Ca2+ and blocked both loss of mitochondrial membrane potential (an indicator of permeability transition pore opening) and apoptosis (assessed by DNA fragmentation). When cytosolic Ca2+ and mitochondrial membrane potential were simultaneously measured by confocal microscopy, sarcoplasmic reticulum (SR)-driven slow Ca2+ oscillations (time-to-peak ∼4 s) were observed in Q209L-expressing cells. These oscillations were seen to transition into sustained increases in cytosolic Ca2+, directly paralleled by loss of mitochondrial membrane potential. Ca2+ transients generated by caffeine-induced release of SR Ca2+ were greatly prolonged in Q209L-expressing cells, suggesting a decreased ability to extrude Ca2+. Indeed, the Na+/Ca2+ exchanger (NCX), which removes Ca2+ from the cell, was markedly down-regulated at the mRNA and protein levels. Adenoviral NCX expression normalized cytosolic Ca2+ levels and prevented DNA fragmentation in cells expressing Q209L. Interestingly, constitutively activated Akt, which rescues cells from Q209L-induced apoptosis, prevented the decrease in NCX expression, normalized cytosolic Ca2+ levels and spontaneous Ca2+ oscillations, shortened caffeine-induced Ca2+ transients, and prevented loss of the mitochondrial membrane potential. Our findings demonstrate that NCX down-regulation and consequent increases in cytosolic and SR Ca2+ can lead to Ca2+ overloading-induced loss of mitochondrial membrane potential and suggest that recovery of Ca2+ dysregulation is a target of Akt-mediated protection. [ABSTRACT FROM AUTHOR]

Published
2005
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44. Akt-mediated Cardiomyocyte Survival Pathways Are Compromised by Gα[sub q]-induced Phosphoinositide 4,5-Biphosphate Depletion.

Author

Howes, Amy L., Arthur, Jane F., Tong Zhang, Miyamoto, Shigeki, Adams, John W., Dorn II, Gerald W., Woodcock, Elizabeth A., and Brown, Joan Heller

Subjects
*PHOSPHOINOSITIDES, *HYPERTROPHY, *PHOSPHORYLATION
Abstract

Expression of the wild type α subunit of G[sub q] (G[sub q]WT) in cardiomyocytes induces hypertrophy, whereas a constitutively active Gα[sub q] subunit (G[sub q]Q209L) induces apoptosis. Akt phosphorylation increases with G[sub q]WT expression but is markedly attenuated in cardiomyocytes expressing G[sub q]Q209L or in those expressing G[sub q]WT and treated with agonist. A membrane-targeted Akt rescues G[sub q]Q209L-expressing cardiomyocytes from apoptotic cell death. In contrast, leukemia inhibitory factor fails to activate Akt or promote cell survival in these cells. Association of Akt and PDK-1 with the membrane is also diminished in G[sub q]Q209L-expressing cardiomyocytes. Phosphatidylinositol 3,4,5-trisphosphate (PIP[sub 3]), the primary regulator of Akt, increases significantly in G[sub q]WT-expressing cells but not in cardiomyocytes expressing G[sub q]Q209L. Levels of phosphatidylinositol 4,5-bisphosphate (PIP[sub 2]), the immediate precursor of PIP[sub 3], are also markedly lower in G[sub q]Q209L-expressing compared to control cells. Expression of a G[sub q]Q209L mutant that has diminished capacity to activate phospholipase C does not decrease PIP[sub 2] or Akt or induce apoptosis. In transgenic mice with cardiac Gα[sub q] overexpression, heart failure and increased cardiomyocyte apoptosis develop during the peripartal period. Akt phosphorylation and PIP[sub 2] levels decrease concomitantly. Our findings suggest that an Akt-mediated cell survival pathway is compromised by the diminished availability of PIP[sub 2] elicited by pathological levels of G[sub q] activity. [ABSTRACT FROM AUTHOR]

Published
2003
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45. Tumor necrosis factor-alpha-stimulated cell proliferation is mediated through sphingosine kinase-dependent Akt activation and cyclin D expression.

Author

Radeff-Huang J, Seasholtz TM, Chang JW, Smith JM, Walsh CT, and Brown JH

Subjects
Brain Neoplasms, Cell Division drug effects, Cell Division physiology, Cell Line, Tumor, Cyclin D, DNA biosynthesis, Enzyme Activation drug effects, Enzyme Activation physiology, Glioblastoma, Humans, Phosphotransferases (Alcohol Group Acceptor) genetics, RNA, Small Interfering, Receptors, Cell Surface metabolism, Receptors, Lysosphingolipid metabolism, Signal Transduction drug effects, Tumor Necrosis Factor-alpha pharmacology, rho GTP-Binding Proteins metabolism, Cyclins metabolism, Phosphotransferases (Alcohol Group Acceptor) metabolism, Proto-Oncogene Proteins c-akt metabolism, Signal Transduction physiology, Tumor Necrosis Factor-alpha metabolism
Abstract

Tumor necrosis factor-alpha (TNF-alpha) has been shown to activate sphingosine kinase (SphK) in a variety of cell types. The extent to which SphK signaling mediates the pleiotropic effects of TNF-alpha is not entirely clear. The current study examined the role of SphK activity in TNF-alpha-stimulated cell proliferation in 1321N1 glioblastoma cells. We first demonstrated that pharmacological inhibitors of SphK markedly decrease TNF-alpha-stimulated DNA synthesis. Signaling mechanisms through which SphK mediated the effect of TNF-alpha on DNA synthesis were then examined. Inhibition of Rho proteins with C3 exoenzyme or of Rho kinase with Y27632 attenuated TNF-alpha-stimulated DNA synthesis. However, RhoA activation by TNF-alpha was not blocked by SphK inhibition. ERK activation was also required for TNF-alpha-stimulated DNA synthesis but likewise TNF-alpha-induced ERK activation was not blocked by inhibition of SphK. Thus, neither RhoA nor ERK activation are the SphK-dependent transducers of TNF-alpha-induced proliferation. In contrast, TNF-alpha-stimulated Akt phosphorylation, which was also required for DNA synthesis, was attenuated by SphK inhibition or SphK1 knockdown by small interfering RNA. Furthermore, cyclin D expression was increased by TNF-alpha in a SphK- and Akt-dependent manner. Additional studies demonstrated that TNF-alpha effects on DNA synthesis, ERK, and Akt phosphorylation are not mediated through cell surface Gi -coupled S1P receptors, because none of these responses were inhibited by pertussis toxin. We conclude that SphK-dependent Akt activation plays a significant role in TNF-alpha-induced cyclin D expression and cell proliferation.

Published
2007
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