Differential susceptibility of naive and differentiated PC-12 cells to methylglyoxal-induced apoptosis: influence of cellular redox

Neuropathologies have been associated with neuronal de-differentiation and oxidative susceptibility. To address whether cellular states determines their oxidative vulnerability, we have challenged naive (undifferentiated) and nerve growth factor-induced differentiated pheochromocytoma (PC12) with me...

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Published in	Current neurovascular research Vol. 2; no. 1; p. 13
Main Authors	Okouchi, Masahiro, Okayama, Naotsuka, Aw, Tak Yee
Format	Journal Article
Language	English
Published	United Arab Emirates 01.01.2005
Subjects	Acetylcysteine - pharmacology Animals Apoptosis - physiology Caspase 3 Caspase 9 Caspases - metabolism Cell Differentiation Enzyme Activation - physiology Glutathione - biosynthesis Ion Channels - physiology Kinetics Mitochondria - physiology Mitochondrial Membrane Transport Proteins Oxidation-Reduction - drug effects PC12 Cells - cytology PC12 Cells - drug effects PC12 Cells - metabolism PC12 Cells - physiology Poly(ADP-ribose) Polymerases - chemistry Pyruvaldehyde - pharmacology Rats
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Abstract	Neuropathologies have been associated with neuronal de-differentiation and oxidative susceptibility. To address whether cellular states determines their oxidative vulnerability, we have challenged naive (undifferentiated) and nerve growth factor-induced differentiated pheochromocytoma (PC12) with methylglyoxal (MG), a model of carbonyl stress. MG dose-dependently induced greater apoptosis (24 h) in naive (nPC12) than differentiated (dPC12) cells. This enhanced nPC12 susceptibility was correlated with a high basal oxidized cellular glutathione-to-glutathione disulfide (GSH/GSSG) redox and an MG-induced GSH-to-Disulfide (GSSG plus protein-bound SSG) imbalance. The loss of redox balance occurred at 30 min post-MG exposure, and was prevented by N-acetylcysteine (NAC) that was unrelated to de novo GSH synthesis. NAC was ineffective when added at 1h post-MG, consistent with an early window of redox signaling. This redox shift was kinetically linked to decreased BcL-2, increased Bax, and release of mitochondrial cytochrome c which preceded caspase-9 and -3 activation and poly ADP-ribose polymerase (PARP) cleavage (1-2 h), consistent with mitochondrial apoptotic signaling. The blockade of apoptosis by cyclosporine A supported an involvement of the mitochondrial permeability transition pore. The enhanced vulnerability of nPC12 cells to MG and its relationship to cellular redox shifts will have important implications for understanding differential oxidative vulnerability in various cell types and their transition states.
AbstractList	Neuropathologies have been associated with neuronal de-differentiation and oxidative susceptibility. To address whether cellular states determines their oxidative vulnerability, we have challenged naive (undifferentiated) and nerve growth factor-induced differentiated pheochromocytoma (PC12) with methylglyoxal (MG), a model of carbonyl stress. MG dose-dependently induced greater apoptosis (24 h) in naive (nPC12) than differentiated (dPC12) cells. This enhanced nPC12 susceptibility was correlated with a high basal oxidized cellular glutathione-to-glutathione disulfide (GSH/GSSG) redox and an MG-induced GSH-to-Disulfide (GSSG plus protein-bound SSG) imbalance. The loss of redox balance occurred at 30 min post-MG exposure, and was prevented by N-acetylcysteine (NAC) that was unrelated to de novo GSH synthesis. NAC was ineffective when added at 1h post-MG, consistent with an early window of redox signaling. This redox shift was kinetically linked to decreased BcL-2, increased Bax, and release of mitochondrial cytochrome c which preceded caspase-9 and -3 activation and poly ADP-ribose polymerase (PARP) cleavage (1-2 h), consistent with mitochondrial apoptotic signaling. The blockade of apoptosis by cyclosporine A supported an involvement of the mitochondrial permeability transition pore. The enhanced vulnerability of nPC12 cells to MG and its relationship to cellular redox shifts will have important implications for understanding differential oxidative vulnerability in various cell types and their transition states.
Author	Okouchi, Masahiro Okayama, Naotsuka Aw, Tak Yee
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SubjectTerms	Acetylcysteine - pharmacology Animals Apoptosis - physiology Caspase 3 Caspase 9 Caspases - metabolism Cell Differentiation Enzyme Activation - physiology Glutathione - biosynthesis Ion Channels - physiology Kinetics Mitochondria - physiology Mitochondrial Membrane Transport Proteins Oxidation-Reduction - drug effects PC12 Cells - cytology PC12 Cells - drug effects PC12 Cells - metabolism PC12 Cells - physiology Poly(ADP-ribose) Polymerases - chemistry Pyruvaldehyde - pharmacology Rats
Title	Differential susceptibility of naive and differentiated PC-12 cells to methylglyoxal-induced apoptosis: influence of cellular redox
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