Mitogen-activated protein kinases mediate changes in gene expression, but not cytoskeletal organization associated with cardiac muscle cell hypertrophy.

Thorburn, Jacqueline; Frost, Jeffrey A.; Thorburn, Andrew

doi:10.1083/jcb.126.6.1565

Cited by 191 publications

(109 citation statements)

References 46 publications

(47 reference statements)

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“…These data confirm that expression from all the promoters, including ANF and MLC-2, is inhibited when ERK activity is blocked, although it remains possible that other MAP kinase family members that are also inhibited by CL100 may play a role in activation of these promoters. Combined with the data from the experiments shown in Figure 2 and our previous studies (Thorburn et al, 1994a), we suggest that ERK activation is required for expression from the Fos, ANF, and MLC-2 promoters, and that ERK activation by MKK is sufficient to induce expression from the Fos promoter but not the ANF or MLC-2 promoters.…”

Section: Materials and Methods Cell Culture And Transfectionssupporting

confidence: 79%

“…Expression of dominant-negative ERK1 or the ERK phosphatase CL100, prevents phenylephrine-induced expression from the ANF or MLC-2 promoters ( Figure 3; Thorburn et al, 1994a). Dominant-negative ERK1 also prevents Raf-l-induced expression (Thorburn et al, 1994b), suggesting that the Raf-1 -> MKK --ERK pathway must be active for expression to occur.…”

Section: Discussionmentioning

confidence: 97%

“…These data indicate that not all phenotypes associated with active Raf-1 are necessarily also associated with active MKK. (Thorburn et al, 1994a Figure 2 indicate that the ANF and MLC-2 promoters respond differently from the Fos promoter and APl-driven genes to expression of the ERK activator MKK. We therefore wished to use a different approach to confirm the requirement for activity of the ERKs for expression from the cardiac-specific promoters.…”

Section: Materials and Methods Cell Culture And Transfectionsmentioning

confidence: 99%

“…Previously, we found that introduction of active Ras or active Raf-1 were each necessary and sufficient for expression from the c-Fos, ANF, and MLC-2 promoters in phenylephrine-induced hypertrophy (Thorburn et al, 1993;Thorburn et al, 1994b). Active MAP kinase is also required for induction by phenylephrine (Thorburn et al, 1994a) or Raf-1 (Thorburn et al, 1994b). Phenylephrine and other hypertrophic agonists cause biochemical activation of Ras , Raf-1 (Thorburn and Thorburn, unpublished data), MKK (Bogoyevitch et al, 1993;Lazou et al, 1994), and ERKs (Bogoyevitch et al, 1993Yamazaki et al, 1993;Thorburn et al, 1994a).…”

Section: Introductionmentioning

confidence: 99%

“…Active MAP kinase is also required for induction by phenylephrine (Thorburn et al, 1994a) or Raf-1 (Thorburn et al, 1994b). Phenylephrine and other hypertrophic agonists cause biochemical activation of Ras , Raf-1 (Thorburn and Thorburn, unpublished data), MKK (Bogoyevitch et al, 1993;Lazou et al, 1994), and ERKs (Bogoyevitch et al, 1993Yamazaki et al, 1993;Thorburn et al, 1994a). In addition, dominantnegative Ras or Raf mutants prevent phenylephrineinduced ERK activation (Thorburn, 1994).…”

Section: Introductionmentioning

confidence: 99%

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Inhibition of a signaling pathway in cardiac muscle cells by active mitogen-activated protein kinase kinase.

Thorburn

Carlson

Mansour

et al. 1995

MBoC

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Signaling via the Ras pathway involves sequential activation of Ras, Raf-1, mitogenactivated protein kinase kinase (MKK), and the extracellular signal-regulated (ERK) group of mitogen-activated protein (MAP) kinases. Expression from the c-Fos, atrial natriuretic factor (ANF), and myosin light chain-2 (MLC-2) promoters during phenylephrine-induced cardiac muscle cell hypertrophy requires activation of this pathway. Furthermore, constitutively active Ras or Raf-1 can mimic the action of phenylephrine in inducing expression from these promoters. In this study, we tested whether constitutively active MKK, the molecule immediately downstream of Raf, was sufficient to induce expression. Expression of constitutively active MKK induced ERK2 kinase activity and caused expression from the c-Fos promoter, but did not significantly activate expression of reporter genes under the control of either the ANF or MLC-2 promoters. Expression of CL100, a phosphatase that inactivates ERKs, prevented expression from all of the promoters. Taken together, these data suggest that ERK activation is required for expression from the Fos, ANF, and MLC-2 promoters but MKK and ERK activation is sufficient for expression only from the Fos promoter. Constitutively active MKK synergized with phenylephrine to increase expression from a c-Fos-or an APi-driven reporter. However, active MKK inhibited phenylephrine-and Raf-1-induced expression from the ANF and MLC-2 promoters. A DNA sequence in the MLC-2 promoter that is a target for inhibition by active MKK, but not CL100, was mapped to a previously characterized DNA element (HF1) that is responsible for cardiac specificity. Thus, activation of cardiac gene expression during phenylephrine-induced hypertrophy requires ERK activation but constitutive activation by MKK can inhibit expression by targeting a DNA element that controls the cardiac specificity of gene expression.

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Section: Materials and Methods Cell Culture And Transfectionssupporting

confidence: 79%

Section: Discussionmentioning

confidence: 97%

Section: Materials and Methods Cell Culture And Transfectionsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Inhibition of a signaling pathway in cardiac muscle cells by active mitogen-activated protein kinase kinase.

Thorburn

Carlson

Mansour

et al. 1995

MBoC

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Inhibition of phenylephrine‐induced cardiac hypertrophy by docosahexaenoic acid

Siddiqui

Shaikh

Kovacs

et al. 2004

J of Cellular Biochemistry

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Many of the cardiovascular benefits of fish oil result from the antiarrhythmic actions of the n-3 polyunsaturated lipids docosahexaenoic acid (DHA) and eicosapentaenoic acid (EPA). The beneficial effects of DHA/EPA in patients with coronary artery disease and myocardial infarction may also result from modulation of the myocardial hypertrophic response. Hypertrophy was assessed in neonatal cardiomyocytes exposed to phenylephrine (PE) by measuring cell surface area, total protein synthesis ((14)C leucine incorporation), and the organization of sarcomeric alpha-actinin and by monitoring expression of atrial natriuretic factor (ANF). We report that PE induced a twofold increase in cell surface area and protein synthesis in cardiomyocytes. The hypertrophied cardiomyocytes also exhibited increased expression of ANF in perinuclear regions and organization of sarcomeric alpha-actinin into classical z-bands. Treatment of cardiomyocytes with 5 microM DHA effectively prevented PE-induced hypertrophy as shown by inhibition of surface area expansion and protein synthesis, inhibition of ANF expression, and prevention of alpha-actinin organization into z-bands. DHA treatment prevented PE-induced activation of Ras and Raf-1 kinase. The upstream inhibition of Ras --> Raf-1 effectively prevented translocation and nuclear localization of phosphorylated extracellularly regulated kinase 1 and 2 (Erk1/2). These effects consequently led to inhibition of nuclear translocation, and hence, activation of the downstream signaling enzyme p90 ribosomal S6 kinase (p90(rsk)). These results indicate that PE-induced cardiac hypertrophy can be minimized by DHA. Our results suggest that inhibition of Ras --> Raf-1 --> Erk1/2 --> p90(rsk) --> hypertrophy is one possible pathway by which DHA can inhibit cardiac hypertrophy. In vivo studies are needed to confirm these in vitro effects of DHA.

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Baicalein protects against cardiac hypertrophy through blocking MEK‐ERK1/2 signaling

Zong

Zhang

Zhou

et al. 2013

J of Cellular Biochemistry

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Baicalein, a flavonoid present in the root of Scutellaria baicalensis, is well known for its antibacterial, antiviral, anti-inflammatory, antithrombotic, and antioxidant effects. Here we show that baicalein also attenuates cardiac hypertrophy. Aortic banding (AB) was performed to induce cardiac hypertrophy secondary to pressure overload in mice. Mouse chow containing 0.05% baicalein (dose: 100 mg/kg/day baicalein) was begun 1 week prior to surgery and continued for 8 weeks after surgery. Our data demonstrated that baicalein prevented cardiac hypertrophy and fibrosis induced by AB, as assessed by echocardiographic and hemodynamic parameters and by pathological and molecular analysis. The inhibitory action of baicalein on cardiac hypertrophy was mediated by effects on mitogen-activated protein kinase kinase (MEK)-extracellular signal-regulated kinases (ERK1/2) signaling and GATA-4 activation. In vitro studies performed in rat cardiac H9c2 cells confirmed that baicalein attenuated cardiomyocyte hypertrophy induced by angiotensin II, which was associated with inhibiting MEK-ERK1/2 signaling. In conclusion, our results suggest that baicalein has protective potential for targeting cardiac hypertrophy and fibrosis through suppression of MEK-ERK1/2 signaling. Baicalein warrants further research as a potential antihypertrophic agent that might be clinically useful to treat cardiac hypertrophy and heart failure.

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Mitogen-activated protein kinases mediate changes in gene expression, but not cytoskeletal organization associated with cardiac muscle cell hypertrophy.

Cited by 191 publications

References 46 publications

Inhibition of a signaling pathway in cardiac muscle cells by active mitogen-activated protein kinase kinase.

Inhibition of a signaling pathway in cardiac muscle cells by active mitogen-activated protein kinase kinase.

Inhibition of phenylephrine‐induced cardiac hypertrophy by docosahexaenoic acid

Baicalein protects against cardiac hypertrophy through blocking MEK‐ERK1/2 signaling

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