G-proteins in growth and apoptosis: lessons from the heart

Adams, John W.; Brown, Joan Heller

doi:10.1038/sj.onc.1204275

Cited by 107 publications

(68 citation statements)

References 107 publications

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“…Similarly, the various signaling pathways activated by AII have all been implicated in cardiac hypertrophy, apoptosis, or both (1,24,46). Their importance in mediating specific AII effects as well as their involvement in AII regulation of cardiac genes has not been firmly elucidated.…”

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confidence: 99%

Convergence of Protein Kinase C and JAK-STAT Signaling on Transcription Factor GATA-4

Wang

Paradis

Aries

et al. 2005

Molecular and Cellular Biology

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Angiotensin II (AII), a potent vasoactive hormone, acts on numerous organs via G-protein-coupled receptors and elicits cell-specific responses. At the level of the heart, AII stimulation alters gene transcription and leads to cardiomyocyte hypertrophy. Numerous intracellular signaling pathways are activated in this process; however, which of these directly link receptor activation to transcriptional regulation remains undefined. We used the atrial natriuretic factor (ANF) gene (NPPA) as a marker to elucidate the signaling cascades involved in AII transcriptional responses. We show that ANF transcription is activated directly by the AII type 1 receptor and precedes the development of myocyte hypertrophy. This response maps to STAT and GATA binding sites, and the two elements transcriptionally cooperate to mediate signaling through the JAK-STAT and protein kinase C (PKC)-GATA-4 pathways. PKC phosphorylation enhances GATA-4 DNA binding activity, and STAT-1 functionally and physically interacts with GATA-4 to synergistically activate AII and other growth factor-inducible promoters. Moreover, GATA factors are able to recruit STAT proteins to target promoters via GATA binding sites, which are sufficient to support synergy. Thus, STAT proteins can act as growth factor-inducible coactivators of tissue-specific transcription factors. Interactions between STAT and GATA proteins may provide a general paradigm for understanding cell specificity of cytokine and growth factor signaling.

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confidence: 99%

Convergence of Protein Kinase C and JAK-STAT Signaling on Transcription Factor GATA-4

Wang

Paradis

Aries

et al. 2005

Molecular and Cellular Biology

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“…Hypertrophy in response to pressure overload involves heterotrimeric G proteins of the G q/11 class (1) and activation of G q is sufficient to cause hypertrophy in vivo (2), as well as in cell models (3). In keeping with this, activation of G q -coupled receptors including ␣ 1 -adrenergic receptors (␣ 1 -AR), 1 ET A receptors or AT 1 receptors on neonatal rat ventricular myocytes (NRVM) causes increased growth of the cardiomyocytes, as well as increasing transcription from "hypertrophic" marker genes, such as ANP and MLC2 (3). Signaling pathways associated with increased protein synthesis, and hence cell size, are known to be partly independent of those causing re-expression of ANP and MLC2, but both can be activated by G q (4).…”

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confidence: 99%

UTP Transactivates Epidermal Growth Factor Receptors and Promotes Cardiomyocyte Hypertrophy Despite Inhibiting Transcription of the Hypertrophic Marker Gene, Atrial Natriuretic Peptide

Morris

Pham

Kenney

et al. 2004

Journal of Biological Chemistry

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In neonatal rat ventricular myocytes, activation of receptors that couple to the G q family of heterotrimeric G proteins causes hypertrophic growth, together with expression of "hypertrophic marker" genes, such as atrial natriuretic peptide (ANP) and myosin light chain 2 (MLC2). As reported previously for other G q -coupled receptors, stimulation of ␣ 1 -adrenergic receptors with phenylephrine (50 M) caused phosphorylation of epidermal growth factor (EGF) receptors as well as activation of ERK1/2, cellular growth, and ANP transcription. These responses depended on EGF receptor activation. In marked contrast, stimulation of G q -coupled purinergic receptors with UTP caused EGF receptor phosphorylation, ERK1/2 activation, and cellular growth but minimal increases in ANP transcription. UTP inhibited phenylephrine-dependent transcription from ANP and MLC2 promoters but not transcription from myoglobin promoters or from AP-1 elements. Myocardin is a muscle-specific transcription enhancer that activates transcription from ANP and MLC2 promoters but not myoglobin promoters or AP-1 elements. UTP inhibited ANP and MLC2 responses to overexpressed myocardin but did not inhibit responses to c-Jun, GATA4, or serum response factor, all of which are active in nonmuscle cells. Thus, UTP inhibits transcriptional responses to phenylephrine only at cardiac-specific promoters, and this may involve the muscle-specific transcription enhancer, myocardin. These studies show that EGF receptor activation is necessary but not sufficient for ANP and MLC2 responses to activation of G q -coupled receptors in ventricular myocytes, because inhibitory mechanisms can oppose such stimulation. ANP is a compensatory and protective factor in cardiac hypertrophy, and mechanisms that reduce its generation need to be defined.

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“…G␣ q/11 is a well-established mediator of cardiac hypertrophy, 10 so we hypothesized that G-protein coupling to the Figure 4A). 17 [Y215F]AT 1 was confirmed as a G proteinuncoupled mutant with robust expression ( Figure S2 and Table S1) and, although [Y215F]AT 1 was described previously with reduced radioligand affinity, we found no statistically significant difference in affinity compared with WT, and the Ang II concentrations used herein are sufficient to ensure almost complete receptor occupancy at either receptor.…”

Section: G-protein Coupling Is Required For Egfr Transactivation and mentioning

confidence: 99%

“…Recent studies suggested a G protein-independent pathway for growth activation, 6 -9 despite evidence that G␣ q/11 , a heterotrimeric G protein that couples to the AT 1 R, is essential for hypertrophy. 10 Indeed, others indicate that G-protein coupling to AT 1 R is required for EGFR transactivation in COS-7 and vascular smooth muscle cells. [11][12][13] Meanwhile, evidence for ␤-arrestin-dependent functional selectivity of the Ang II analog sarcosine, 1 isoleucine, 4 isoleucine, 8 Ang II (SII Ang II), 14 ␤-arrestin-mediated EGFR transactivation by ␤ 1 -adrenoceptors independent of G-protein coupling, 15 and the very recent demonstration of ␤-arrestin-dependent hypertrophy resulting from mechanical stretch 16 suggests that ␤-arrestin scaffolding of extracellular signal-regulated kinase (ERK) 1/2 may contribute to transactivation and/or cardiac hypertrophy.…”

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confidence: 99%

Determination of the Exact Molecular Requirements for Type 1 Angiotensin Receptor Epidermal Growth Factor Receptor Transactivation and Cardiomyocyte Hypertrophy

et al. 2011

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Abstract-Major interest surrounds how angiotensin II triggers cardiac hypertrophy via epidermal growth factor receptor transactivation. G protein-mediated transduction, angiotensin type 1 receptor phosphorylation at tyrosine 319, and ␤-arrestin-dependent scaffolding have been suggested, yet the mechanism remains controversial. We examined these pathways in the most reductionist model of cardiomyocyte growth, neonatal ventricular cardiomyocytes. Analysis with [ 32 P]-labeled cardiomyocytes, wild-type and [Y319A] angiotensin type 1 receptor immunoprecipitation and phosphorimaging, phosphopeptide analysis, and antiphosphotyrosine blotting provided no evidence for tyrosine phosphorylation at Y319 or indeed of the receptor, and mutation of Y319 (to A/F) did not prevent either epidermal growth factor receptor transactivation in COS-7 cells or cardiomyocyte hypertrophy. Instead, we demonstrate that transactivation and cardiomyocyte hypertrophy are completely abrogated by loss of G-protein coupling, whereas a constitutively active angiotensin type 1 receptor mutant was sufficient to trigger transactivation and growth in the absence of ligand. These results were supported by the failure of the ␤-arrestin-biased ligand SII angiotensin II to transactivate epidermal growth factor receptor or promote hypertrophy, whereas a ␤-arrestin-uncoupled receptor retained these properties. We also found angiotensin II-mediated cardiomyocyte hypertrophy to be attenuated by a disintegrin and metalloprotease inhibition. Thus, G-protein coupling, and not Y319 phosphorylation or ␤-arrestin scaffolding, is required for epidermal growth factor receptor transactivation and cardiomyocyte hypertrophy via the angiotensin type 1 receptor. A ngiotensin II (Ang II) contributes to progression of left ventricular hypertrophy, a major independent risk factor for myocardial infarction and sudden death, 1 yet the molecular mechanisms governing cardiac hypertrophy remain controversial. Recently, a new paradigm for Ang II hypertrophy has emerged. We and others have shown that angiotensin type 1 receptors (AT 1 Rs) hijack the epidermal growth factor (EFR) receptor (EGFR) via a process termed the "triple membrane-passing signaling paradigm of EGFR transactivation." 2-5 More specifically, AT 1 R activation causes metalloprotease-dependent EGF-like ligand release and subsequent EGFR binding to initiate hypertrophic signaling cascades. Yet the process is likely more complicated: multiple G protein-coupled receptor (GPCR) signals, a disintegrin and metalloproteases (ADAMs), EGF-like ligands, and EGFR subtypes have been implicated in this process. 2 A major focus of Ang II research is the mechanism by which the AT 1 R signals to the EGFR. Recent studies suggested a G protein-independent pathway for growth activation, 6 -9 despite evidence that G␣ q/11 , a heterotrimeric G protein that couples to the AT 1 R, is essential for hypertrophy. 10 Indeed, others indicate that G-protein coupling to AT 1 R is required for EGFR transactivation in COS-7 and vascular smoot...

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G-proteins in growth and apoptosis: lessons from the heart

Cited by 107 publications

References 107 publications

Convergence of Protein Kinase C and JAK-STAT Signaling on Transcription Factor GATA-4

Convergence of Protein Kinase C and JAK-STAT Signaling on Transcription Factor GATA-4

UTP Transactivates Epidermal Growth Factor Receptors and Promotes Cardiomyocyte Hypertrophy Despite Inhibiting Transcription of the Hypertrophic Marker Gene, Atrial Natriuretic Peptide

Determination of the Exact Molecular Requirements for Type 1 Angiotensin Receptor Epidermal Growth Factor Receptor Transactivation and Cardiomyocyte Hypertrophy

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