Expression, activity, and pro-hypertrophic effects of PDE5A in cardiac myocytes

Zhang, Manling; Koitabashi, Norimichi; Nagayama, Takahiro; Rambaran, Ryan; Feng, Ning; Takimoto, Eiki; Koenke, Trisha; O’Rourke, Brian; Champion, Hunter C.; Crow, Michael T.; Kass, David A.

doi:10.1016/j.cellsig.2008.08.012

Cited by 83 publications

(90 citation statements)

References 34 publications

(62 reference statements)

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“…Inhibition of PDE5 in the hypertrophied myocardium significantly improved myocardial contractility (17). Unlike previous reports, more recent studies have shown that PDE5A was expressed in the cardiomyocytes, and targeted inhibition of its activity with sildenafil modulated the cardiomyocyte hypertrophy response to phenylephrine treatment in vitro (27). Extrapolating these observations of cytoprotective effects to the bone marrow-derived mesenchymal stem cells (MSCs), we hypothesized that inhibition of PDE5A activity with tadalafil would promote cGMP/protein kinase G (PKG) activity to condition stem cells for improved survival and proliferation postengraftment in the infarcted heart.…”

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confidence: 60%

Phosphodiesterase inhibition with tadalafil provides longer and sustained protection of stem cells

Haider

Lee

Jiang

et al. 2010

American Journal of Physiology-Heart and Circulatory Physiology

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We hypothesized that inhibition of the cGMP-specific enzyme phosphodiesterase 5A (PDE5A) promoted cGMP/protein kinase G (PKG) activity to condition stem cells for enhanced survival and proliferation. One-time tadalafil treatment (1 μM for 30 min) of mesenchymal stem cells (TadaMSCs) provided sustained protection of cells for 36 h. Higher cGMP activity with concomitantly increased PKG1 activity was observed inTadaMSCs, which peaked within 12 h after tadalafil treatment. Pretreatment with PKG1 blockers (1 μM KT-5823 or 20 nM K-252a) or transduction with adenoviral PKG1-short-hairpin RNA abolished tadalafil-induced cytoprotection of the cells. A higher proliferation rate was observed inTadaMSCs compared with nontreated MSCs (ContMSCs). In a rat model of acute myocardial infarction,TadaMSCs transplanted 0 and 24 h after tadalafil treatment showed higher survival compared withContMSCs on day 2 and day 4 after engraftment.TadaMSCs transplanted 48 h after tadalafil treatment lost their protection on both day 2 and day 4 after engraftment, and their rate of survival was similar toContMSCs. Reduced terminal dUTP nick end-labeling positivity ( P < 0.01 vs.ContMSCs) and higher proliferation ofTadaMSCs ( P < 0.01 vs.ContMSCs) was observed in the infarcted heart. Fluorescence immunostaining revealed neomyogenesis in both the infarct and peri-infarct areas. Blood vessel density was significantly increased in group 2 compared with group 1. Transthoracic echocardiographic heart function revealed significant preservation of the indexes of left ventricle contractility and attenuation of remodeling inTadaMSC-engrafted animal hearts ( group 2) compared withContMSCs ( group 1). PDE5A inhibition using long-acting tadalafil is an innovative approach to promote stem cell survival and proliferation in the infarcted heart.

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confidence: 60%

Phosphodiesterase inhibition with tadalafil provides longer and sustained protection of stem cells

Haider

Lee

Jiang

et al. 2010

American Journal of Physiology-Heart and Circulatory Physiology

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“…The EmGFP linked to the artificial miRNA region was then transferred into pAd.CMV-DEST by recombinase cloning (Invitrogen). A control adenovirus (Ad.Neg-shRNA) containing EmGFP and a control shRNAmiR that was predicted not to target any known vertebrate gene was reported earlier (54). The initial viral amplification and purification was performed in our laboratory using an AdenopureLS adenovirus purification kit (Puresyn; Malvern, PA) according to the manufacturer's instructions.…”

Section: Methodsmentioning

confidence: 99%

Knockdown of lung phosphodiesterase 2A attenuates alveolar inflammation and protein leak in a two-hit mouse model of acute lung injury

Rentsendorj

Damarla

Aggarwal

et al. 2011

American Journal of Physiology-Lung Cellular and Molecular Phys

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is stimulated by cGMP to hydrolyze cAMP, a potent endothelial barrier-protective molecule. We previously found that lung PDE2A contributed to a mouse model of ventilator-induced lung injury (VILI). The purpose of the present study was to determine the contribution of PDE2A in a two-hit mouse model of 1-day intratracheal (IT) LPS followed by 4 h of 20 ml/kg tidal volume ventilation. Compared with IT water controls, LPS alone (3.75 g/g body wt) increased lung PDE2A mRNA and protein expression by 6 h with a persistent increase in protein through day 4 before decreasing to control levels on days 6 and 10. Similar to the PDE2A time course, the peak in bronchoalveolar lavage (BAL) neutrophils, lactate dehydrogenase (LDH), and protein concentration also occurred on day 4 post-LPS. IT LPS (1 day) and VILI caused a threefold increase in lung PDE2A and inducible nitric oxide synthase (iNOS) and a 24-fold increase in BAL neutrophilia. Compared with a control adenovirus, PDE2A knockdown with an adenovirus expressing a short hairpin RNA administered IT 3 days before LPS/VILI effectively decreased lung PDE2A expression and significantly attenuated BAL neutrophilia, LDH, protein, and chemokine levels. PDE2A knockdown also reduced lung iNOS expression by 53%, increased lung cAMP by nearly twofold, and improved survival from 47 to 100%. We conclude that in a mouse model of LPS/VILI, a synergistic increase in lung PDE2A expression increased lung iNOS and alveolar inflammation and contributed significantly to the ensuing acute lung injury.lipopolysaccharide; ventilator-induced; cyclic guanosine monophosphate; inducible nitric oxide synthase; cAMP SEVERE PNEUMONIA IS A FREQUENT cause of acute lung injury (ALI) and the acute respiratory distress syndrome (ARDS) (49). ARDS is characterized by neutrophil infiltration, the generation of toxic cytokines and reactive oxygen species (ROS), increased NO production and the loss of endothelial and epithelial barrier function (4). These features can be reproduced in animal models by the installation of intratracheal (IT) LPS (10, 24, 31), a key component of the gram-negative bacterial cell wall. LPS, through Toll-like receptor-4 signaling, was shown to cause increased NO from phosphorylated endothelial (eNOS) (11) and inducible nitric oxide synthase (iNOS) (24, 31) in alveolar macrophages, neutrophils, epithelium, and endothelium. NO from both eNOS and iNOS was found to play a major pathogenic role in ALI from LPS (24, 31, 42) and in ventilator-induced lung injury (VILI) (33, 39). These injurious effects of endogenous NO have been attributed to a reaction with superoxide to generate peroxynitrite (31, 33). In both LPS-induced ALI (47) and VILI (39), however, NO also activates soluble guanylyl cyclase (sGC), increasing production of cGMP in multiple cell types including endothelium (39), epithelium (9, 17), and macrophages (3).The effects of cGMP signaling in ALI are complex, depending on cell type, intracellular compartmentalization, and the downstream cGMP targets (39). These targets include...

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“…Second, PDE5 inhibition suppresses Cn/nuclear factor of activated T cell (Cn/NFAT) signaling and expression of the genes encoding atrial and brain natriuretic peptides in isolated myocytes stimulated with a G q agonist (21,44). Third, knockdown of the gene encoding PDE5 in cardiac myocytes is antihypertrophic, having an impact similar to that of sildenafil, and the effect of combining both is similar to that of each alone (44). This last finding supports specificity of sildenafil for inhibiting PDE5.…”

Section: Figurementioning

confidence: 99%

Regulator of G protein signaling 2 mediates cardiac compensation to pressure overload and antihypertrophic effects of PDE5 inhibition in mice

Takimoto¹,

Koitabashi²,

Hsu³

et al. 2009

J. Clin. Invest.

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The heart initially compensates for hypertension-mediated pressure overload by enhancing its contractile force and developing hypertrophy without dilation. G q protein-coupled receptor pathways become activated and can depress function, leading to cardiac failure. Initial adaptation mechanisms to reduce cardiac damage during such stimulation remain largely unknown. Here we have shown that this initial adaptation requires regulator of G protein signaling 2 (RGS2). Mice lacking RGS2 had a normal basal cardiac phenotype, yet responded rapidly to pressure overload, with increased myocardial G q signaling, marked cardiac hypertrophy and failure, and early mortality. Swimming exercise, which is not accompanied by G q activation, induced a normal cardiac response, while Rgs2 deletion in G αq -overexpressing hearts exacerbated hypertrophy and dilation. In vascular smooth muscle, RGS2 is activated by cGMP-dependent protein kinase (PKG), suppressing G q -stimulated vascular contraction. In normal mice, but not Rgs2 -/-mice, PKG activation by the chronic inhibition of cGMP-selective phosphodiesterase 5 (PDE5) suppressed maladaptive cardiac hypertrophy, inhibiting G q -coupled stimuli. Importantly, PKG was similarly activated by PDE5 inhibition in myocardium from both genotypes, but PKG plasma membrane translocation was more transient in Rgs2 -/-myocytes than in controls and was unaffected by PDE5 inhibition. Thus, RGS2 is required for early myocardial compensation to pressure overload and mediates the initial antihypertrophic and cardioprotective effects of PDE5 inhibitors.

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Expression, activity, and pro-hypertrophic effects of PDE5A in cardiac myocytes

Cited by 83 publications

References 34 publications

Phosphodiesterase inhibition with tadalafil provides longer and sustained protection of stem cells

Phosphodiesterase inhibition with tadalafil provides longer and sustained protection of stem cells

Knockdown of lung phosphodiesterase 2A attenuates alveolar inflammation and protein leak in a two-hit mouse model of acute lung injury

Regulator of G protein signaling 2 mediates cardiac compensation to pressure overload and antihypertrophic effects of PDE5 inhibition in mice

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