Glycogen Synthase Kinase 3 Inhibition Slows Mitochondrial Adenine Nucleotide Transport and Regulates Voltage-Dependent Anion Channel Phosphorylation

Das, Samarjit; Wong, Renee; Rajapakse, Nishadi; Murphy, Elizabeth; Steenbergen, Charles

doi:10.1161/circresaha.108.178970

Cited by 174 publications

(186 citation statements)

References 41 publications

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“…To confirm that the dysregulation of cAMP production in the KO mouse was due to a direct effect of deletion of Gsk3a, we used SB415286, a relatively selective, small molecule inhibitor of GSK-3 (25,26). Pretreatment of WT cardiomyocytes for 30 minutes with SB415286 led to a significant reduction in the contractile response to isoproterenol, mimicking the findings in the KO cells ( Figure 8C).…”

Section: Figuresupporting

confidence: 55%

GSK-3α directly regulates β-adrenergic signaling and the response of the heart to hemodynamic stress in mice

Zhou¹,

Lal²,

Chen³

et al. 2010

J. Clin. Invest.

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The glycogen synthase kinase-3 (GSK-3) family of serine/threonine kinases consists of 2 highly related isoforms, α and β. Although GSK-3β has an important role in cardiac development, much remains unknown about the function of either GSK-3 isoform in the postnatal heart. Herein, we present what we believe to be the first studies defining the role of GSK-3α in the mouse heart using gene targeting. Gsk3a -/-mice over 2 months of age developed progressive cardiomyocyte and cardiac hypertrophy and contractile dysfunction. Following thoracic aortic constriction in young mice, we observed enhanced hypertrophy that rapidly transitioned to ventricular dilatation and contractile dysfunction. Surprisingly, markedly impaired β-adrenergic responsiveness was found at both the organ and cellular level. This phenotype was reproduced by acute treatment of WT cardiomyocytes with a small molecule GSK-3 inhibitor, confirming that the response was not due to a chronic adaptation to LV dysfunction. Thus, GSK-3α appears to be the central regulator of a striking range of essential processes, including acute and direct positive regulation of β-adrenergic responsiveness. In the absence of GSK-3α, the heart cannot respond effectively to hemodynamic stress and rapidly fails. Our findings identify what we believe to be a new paradigm of regulation of β-adrenergic signaling and raise concerns given the rapid expansion of drug development targeting GSK-3.

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Section: Figuresupporting

confidence: 55%

GSK-3α directly regulates β-adrenergic signaling and the response of the heart to hemodynamic stress in mice

Zhou¹,

Lal²,

Chen³

et al. 2010

J. Clin. Invest.

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“…GSK-3b inhibition), which protects the adult-rat heart from I/R injury for 2-4 h. 4,[13][14][15][16] This study showed a link between the Zn 2 þ i release/increase and the activation of GSK-3b, resulting in myocyte apoptosis. We observed an early increase in p-Ser9 GSK-3b levels after Zn 2 þ Figure S2b), we conclude that Zn 2 þ i supplementation-induced early phosphorylation at Ser9 is not necessarily cardioprotective and may induce cytotoxicity after return to normal medium for 4 or 24 h. In support of the above conclusions, Tyr216 phosphorylation is required for nuclear GSK-3b accumulation in neurons and fibroblasts, 17,18 as mutation of Tyr216 to phenylalanine or its dephosphorylation results in less GSK-3b being found in nuclei.…”

Section: Discussionmentioning

confidence: 67%

“…When the reperfusion injury salvage kinase (RISK) family members PKA, PKB/Akt, PKC, and MEK-ERK are activated by pre-or post-conditioning, a common downstream protein, GSK-3b, is phosphorylated at Ser9, resulting in GSK-3b inhibition (both events occurring within 20 min of the end of conditioning), leading to the inhibition of mPTPs and the salvaging of 20-50% live myocardium. 4,5,[13][14][15][16] A potent GSK-3 inhibitor, SB216763 (SB21), 4,13 had a relatively weak protective effect against H 2 O 2 -, ONOO À -induced myocyte death (Supplementary Figure S2c), but gave better protection against 10 mM Zn 2 þ -induced cell toxicity at 4 h (Figure 2d (TUNEL test) were performed as follows: after ischemia for 40 min, followed by reperfusion for 4 h, myocytes were returned to normal medium without inhibitors for 24 h, then were examined for apoptotic markers. Compared with I/R alone ('I/R', Figure 4b), the presence of 15 mM TPEN at the start of reperfusion for only B20 min ('TPEN (20 min)') markedly inhibited I/R injury at 24 h after TPEN removal, suggesting that the reperfusion-induced initial Zn 2 þ i release (Figure 3b) is important in I/R injury.…”

Section: Resultsmentioning

confidence: 99%

“…In contrast, when Zn 2 þ /pyrithione was added for only B20 min at the beginning of reperfusion, it had little protective effect for both cardiomyocytes and H9c2 cells (Figures 4a and b; Supplementary Figures S2a and b). Inclusion of any of three potent flavonoids or U0126 for 4 h in the reperfusion solution again had a marked cardioprotective effect for at least 24 h (Figures 4a and b; Supplementary Figures S2a and b), while Ca 2 þ -free medium (inhibition of I/R-induced Ca 2 þ i overload), 5 CsA (an mPTP inhibitor), 13 diazoxide (an mK ATP opener), 7 or MK886 (a selective 5-LOX inhibitor 8 ) were less protective (Figures 4a and b).…”

Section: Resultsmentioning

confidence: 99%

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Intracellular zinc release-activated ERK-dependent GSK-3β–p53 and Noxa–Mcl-1 signaling are both involved in cardiac ischemic-reperfusion injury

et al. 2011

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“…Indeed, the impact of charge modification on VDAC channel function has been shown previously as VDAC treatment with succinic anhydride, which increases the negative charge of the channel, eliminates VDAC voltage-dependence and changes its selectivity from anion to cation (79). Further, VDAC phosphorylation leading to increased negative charge was shown to decrease the conductance of the channel, though the modified residue(s) were not identified (80,81). It is also possible that the association of VDAC with modulatory proteins is altered when VDAC is succinated; an increase in the negative charge of the protein could e.g.…”

Section: Protein Succination In Leigh Syndromementioning

confidence: 95%

Succination is Increased on Select Proteins in the Brainstem of the NADH dehydrogenase (ubiquinone) Fe-S protein 4 (Ndufs4) Knockout Mouse, a Model of Leigh Syndrome

Piroli

Manuel

Clapper

et al. 2016

Molecular & Cellular Proteomics

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Elevated fumarate concentrations as a result of Krebs cycle inhibition lead to increases in protein succination, an irreversible post-translational modification that occurs when fumarate reacts with cysteine residues to generate S-(2-succino)cysteine (2SC). Metabolic events that reduce NADH re-oxidation can block Krebs cycle activity; therefore we hypothesized that oxidative phosphorylation deficiencies, such as those observed in some mitochondrial diseases, would also lead to increased protein succination. Using the Ndufs4 knockout (Ndufs4 KO) mouse, a model of Leigh syndrome, we demonstrate for the first time that protein succination is increased in the brainstem (BS), particularly in the vestibular nucleus. Importantly, the brainstem is the most affected region exhibiting neurodegeneration and astrocyte and microglial proliferation, and these mice typically die of respiratory failure attributed to vestibular nucleus pathology. In contrast, no increases in protein succination were observed in the skeletal muscle, corresponding with the lack of muscle pathology observed in this model. 2D SDS-PAGE followed by immunoblotting for succinated proteins and MS/MS analysis of BS proteins allowed us to identify the voltagedependent anion channels 1 and 2 as specific targets of succination in the Ndufs4 knockout. Using targeted mass spectrometry, Cys 77 and Cys 48 were identified as endogenous sites of succination in voltage-dependent anion channels 2. Given the important role of voltage-dependent anion channels isoforms in the exchange of ADP/ATP between the cytosol and the mitochondria, and the already decreased capacity for ATP synthesis in the Ndufs4 KO mice, we propose that the increased protein succination observed in the BS of these animals would further decrease the already compromised mitochondrial function. These data suggest that fumarate is a novel bio- We previously identified the formation of S-(2-succino)cysteine (2SC) 1 (protein succination) as a result of the irreversible reaction of fumarate with reactive cysteine thiols (1, 2). Fumarate concentrations are increased during adipogenesis and adipocyte maturation (2,3), and the excess of glucose and insulin leads to augmented protein succination in the adipose tissue of type 2 diabetic mice (4, 5). Protein succination is also specifically increased in fumarate hydratase deficient hereditary leiomyomatosis and renal cell carcinoma (HLRCC), because of the decreased conversion of fumarate to malate (6, 7). In both cases, intracellular fumarate concentrations are elevated; in fumarate hydratase deficient cells, the fumarate concentration is about 5 mM (8) Author contributions: G.G.P. and N.F. designed research; G.G.P., A.M.M., A.C.C., M.D.W., J.E.B., A.Q., and N.F. performed research; J.E.B., R.D.P., and A.Q. contributed new reagents or analytic tools; G.G.P., A.M.M., M.D.W., J.E.B., and N.F. analyzed data; G.G.P. and N.F. wrote the paper. 1 The abbreviations used are: 2SC, S-(2-succino)cysteine; 2D, twodimensional; BS, brainstem; CB, cerebellum; C PE , cystei...

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Glycogen Synthase Kinase 3 Inhibition Slows Mitochondrial Adenine Nucleotide Transport and Regulates Voltage-Dependent Anion Channel Phosphorylation

Cited by 174 publications

References 41 publications

GSK-3α directly regulates β-adrenergic signaling and the response of the heart to hemodynamic stress in mice

GSK-3α directly regulates β-adrenergic signaling and the response of the heart to hemodynamic stress in mice

Intracellular zinc release-activated ERK-dependent GSK-3β–p53 and Noxa–Mcl-1 signaling are both involved in cardiac ischemic-reperfusion injury

Succination is Increased on Select Proteins in the Brainstem of the NADH dehydrogenase (ubiquinone) Fe-S protein 4 (Ndufs4) Knockout Mouse, a Model of Leigh Syndrome

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