Activation of HuR downstream of p38 MAPK promotes cardiomyocyte hypertrophy

Slone, Samuel; Anthony, Sarah; Wu, Xiaoqing; Benoit, Joshua B.; Aubé, Jeffrey; Xu, Liang; Tranter, Michael

doi:10.1016/j.cellsig.2016.08.005

Cited by 42 publications

(42 citation statements)

References 28 publications

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“…Because PKC is not involved in AVP release induced by ANGII, it is reasonable to suggest that the activation of p38 MAPK can be PKC independent. Indeed, recent studies have reported PKC-independent p38 MAPK activation in some tissues (Lemonnier et al 2004, Samuvel et al 2005, Slone et al 2016. Moreover, we observed that E2 prevented the ANGII-induced p38 MAPK phosphorylation in the PVN and the SON, which can explain the inhibitory effect of E2 on ANGII-induced OT and AVP secretion.…”

Section: Figuresupporting

confidence: 69%

17β-Estradiol attenuates p38MAPK activity but not PKCα induced by angiotensin II in the brain

Almeida-Pereira

Vilhena‐Franco

Coletti

et al. 2019

Journal of Endocrinology

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17β-Estradiol (E2) has been shown to modulate the renin–angiotensin system in hydromineral and blood pressure homeostasis mainly by attenuating angiotensin II (ANGII) actions. However, the cellular mechanisms of the interaction between E2 and angiotensin II (ANGII) and its physiological role are largely unknown. The present experiments were performed to better understand the interaction between ANGII and E2 in body fluid control in female ovariectomized (OVX) rats. The present results are the first to demonstrate that PKC/p38 MAPK signaling is involved in ANGII-induced water and sodium intake and oxytocin (OT) secretion in OVX rats. In addition, previous data from our group revealed that the ANGII-induced vasopressin (AVP) secretion requires ERK1/2 signaling. Therefore, taken together, the present observations support a novel concept that distinct intracellular ANGII signaling gives rise to distinct neurohypophyseal hormone release. Furthermore, the results show that E2 attenuates p38 MAPK phosphorylation in response to ANGII but not PKC activity in the hypothalamus and the lamina terminalis, suggesting that E2 modulates ANGII effects through the attenuation of the MAPK pathway. In conclusion, this work contributes to the further understanding of the interaction between E2 and ANGII signaling in hydromineral homeostasis, as well as it contributes to further elucidate the physiological relevance of PKC/p38 MAPK signaling on the fluid intake and neurohypophyseal release induced by ANGII.

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Section: Figuresupporting

confidence: 69%

17β-Estradiol attenuates p38MAPK activity but not PKCα induced by angiotensin II in the brain

Almeida-Pereira

Vilhena‐Franco

Coletti

et al. 2019

Journal of Endocrinology

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“…While relatively little is known about the role of HuR in the myocardium, RNA binding proteins such as HuR are becoming recognized as potentially central regulators of cardiac physiology and pathology (6,7). We have recently shown that HuR is both necessary and sufficient for hypertrophic growth in cultured primary rat myocytes in response to hypertrophic stimuli in vitro (8).…”

Section: Introductionmentioning

confidence: 99%

Human antigen R as a therapeutic target in pathological cardiac hypertrophy

Green¹,

Anthony²,

Slone³

et al. 2019

JCI Insight

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“…In fact, HuR was previously reported to promote translation of target mRNAs by interacting with IRES sequences located in the 59 UTR (94,95). Moreover, HuR can be activated by p38 MAPK to stabilize target mRNAs (56,(96)(97)(98) and in this context, Farooq et al (56) showed that HuR is required for the survival motor neuron protein increase seen in celecoxib-treated NT2 cells. In our work, we observed that celecoxib induced a marked ;2and 4-fold increase in HuR protein levels in TA and DIA muscles, respectively (Supplemental Fig.…”

Section: Celecoxib Treatment Stimulates Utrophin a Expression In Skelmentioning

confidence: 97%

Celecoxib treatment improves muscle function in mdx mice and increases utrophin A expression

2018

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Duchenne muscular dystrophy (DMD) is a genetic and progressive neuromuscular disorder caused by mutations and deletions in the dystrophin gene. Although there is currently no cure, one promising treatment for DMD is aimed at increasing endogenous levels of utrophin A to compensate functionally for the lack of dystrophin. Recent studies from our laboratory revealed that heparin treatment of mdx mice activates p38 MAPK, leading to an upregulation of utrophin A expression and improvements in the dystrophic phenotype. Based on these findings, we sought to determine the effects of other potent p38 activators, including the cyclooxygenase (COX)-2 inhibitor celecoxib. In this study, we treated 6-wk-old mdx mice for 4 wk with celecoxib. Immunofluorescence analysis of celecoxib-treated mdx muscles revealed a fiber type switch from a fast to a slower phenotype along with beneficial effects on muscle fiber integrity. In agreement, celecoxib-treated mdx mice showed improved muscle strength. Celecoxib treatment also induced increases in utrophin A expression ranging from ∼1.5- to 2-fold in tibialis anterior diaphragm and heart muscles. Overall, these results highlight that activation of p38 in muscles can indeed lead to an attenuation of the dystrophic phenotype and reveal the potential role of celecoxib as a novel therapeutic agent for the treatment of DMD.-Péladeau, C., Adam, N. J., Jasmin, B. J. Celecoxib treatment improves muscle function in mdx mice and increases utrophin A expression.

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Activation of HuR downstream of p38 MAPK promotes cardiomyocyte hypertrophy

Cited by 42 publications

References 28 publications

17β-Estradiol attenuates p38MAPK activity but not PKCα induced by angiotensin II in the brain

17β-Estradiol attenuates p38MAPK activity but not PKCα induced by angiotensin II in the brain

Human antigen R as a therapeutic target in pathological cardiac hypertrophy

Celecoxib treatment improves muscle function in mdx mice and increases utrophin A expression

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