Overexpression of Heme Oxygenase in Neuronal Cells, the Possible Interaction with Tau

Takeda, Atsushi; Perry, George; Abraham, Nader G.; Dwyer, Barney E.; Kutty, R. Krishnan; Laitinen, Jarmo T.; Petersen, Robert B.; Smith, Mark A.

doi:10.1074/jbc.275.8.5395

Cited by 176 publications

(106 citation statements)

References 38 publications

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“…Therefore, the regulation of tau phosphorylation in the adult mammalian brain appears to represent a naturally occurring process that is associated with neuroprotective mechanisms [70]. In support of this, it has been observed that cellular antioxidant induction and tau expression are opposing [56,72], suggesting that the reduced oxidative damage in neurons showing tau accumulation [73] might be a direct consequence of an antioxidant function of phosphorylated tau [51,54].…”

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confidence: 58%

Tau phosphorylation in Alzheimer's disease: pathogen or protector?

Lee

Perry

Moreira

et al. 2005

Trends in Molecular Medicine

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mentioning

confidence: 58%

Tau phosphorylation in Alzheimer's disease: pathogen or protector?

Lee

Perry

Moreira

et al. 2005

Trends in Molecular Medicine

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212

123

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“…Heme oxygenase-1 (HO-1) is an antioxidant enzyme that degrades heme into biliverdin, iron and carbon monoxide and is one of the most sensitive and selective indicators of the cellular oxidative stress response. It has been shown that brains of AD patients present an increase of both HO-1 mRNA and protein [58,65] which co-localizes and parallels the expression of the altered form of tau characteristic of AD [76,77].…”

Section: −•mentioning

confidence: 99%

Lipoic Acid and N-acetyl Cysteine Decrease Mitochondrial-Related Oxidative Stress in Alzheimer Disease Patient Fibroblasts

Moreira

Harris

Zhu

et al. 2007

JAD

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173

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Abstract. In this study, we evaluated the effect of lipoic acid (LA) and N -acetyl cysteine (NAC) on oxidative [4-hydroxy-2-nonenal, N ε -(carboxymethyl)lysine and heme oxygenase-1] and apoptotic (caspase 9 and Bax) markers in fibroblasts from patients with Alzheimer disease (AD) and age-matched and young controls. AD fibroblasts showed the highest levels of oxidative stress, and the antioxidants, lipoic acid (1 mM) and/or N -acetyl cysteine (100 µM) exerted a protective effect as evidenced by decreases in oxidative stress and apoptotic markers. Furthermore, we observed that the protective effect of LA and NAC was more pronounced when both agents were present simultaneously. AD-type changes could be generated in control fibroblasts using N -methylprotoporphyrin to inhibit cytochrome oxidase assembly indicating that the the oxidative damage observed was associated with mitochondrial dysfunction. The effects of N -methylprotoporphyrine were reversed or attenuated by both lipoic acid and N -acetyl cysteine. These data suggest mitochondria are important in oxidative damage that occurs in AD. As such, antioxidant therapies based on lipoic acid and N -acetyl cysteine supplementation may be promising.

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“…Hsps serve as molecular chaperones and among the various Hsps, Hsp32 (also known as HO-1) and Hsp72 have been recently demonstrated to play neuroprotective role against oxidative stress (20). HO-1 is the inducible form of a group of enzymes that catalyze heme degradation to form the antioxidant biliverdin and CO (22). Overexpression of human HO-1 gene has been shown to result in a stable increase of HO activity associated with neuroprotection against oxidative injury (23).…”

Section: Introductionmentioning

confidence: 99%

Involvement of PI3K/PKG/ERK1/2 signaling pathways in cortical neurons to trigger protection by cotreatment of acetyl-L-carnitine and α-lipoic acid against HNE-mediated oxidative stress and neurotoxicity: Implications for Alzheimer's disease

Abdul

Butterfield

2007

Free Radical Biology and Medicine

126

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Oxidative stress has been shown to underlie neuropathological aspects of Alzheimer's disease (AD). 4-Hydroxy-2-nonenal (HNE) is a highly reactive product of lipid peroxidation of unsaturated lipids. HNE-induced oxidative toxicity is a well-described model of oxidative stress-induced neurodegeneration. GSH plays a key role in antioxidant defense, and HNE exposure causes an initial depletion of GSH that leads to gradual toxic accumulation of reactive oxygen species. In the current study, we investigated whether pre-treatment of cortical neurons with acetyl-L-carnitine (ALCAR) and α-lipoic acid (LA) plays a protective role in cortical neuronal cells against HNE-mediated oxidative stress and neurotoxicity. Decreased cell survival of neurons treated with HNE correlated with increased protein oxidation (protein carbonyl, 3-nitrotyrosine) and lipid peroxidation (HNE) accumulation. Pretreatment of primary cortical neuronal cultures with ALCAR and LA significantly attenuated HNE-induced cytotoxicity, protein oxidation, lipid peroxidation and apoptosis in a dosedependent manner. Additionally, pretreatment of ALCAR and LA also led to elevated cellular GSH and heat shock proteins (HSPs) levels compared to untreated control cells. We have also determined that pretreatment of neurons with ALCAR and LA leads to the activation of phosphoinositol-3 kinase (PI3K), PKG and ERK1/2 pathways, which play essential roles in neuronal cell survival. Thus, this study demonstrates a cross talk between the PI3K, PKG and ERK1/2 pathways in cortical neuronal cultures that contributes to ALCAR and LA-mediated pro-survival signaling mechanisms. This evidence supports the pharmacological potential of co-treatment of ALCAR and LA in the management of neurodegenerative disorders associated with HNE-induced oxidative stress and neurotoxicity, including AD.

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Overexpression of Heme Oxygenase in Neuronal Cells, the Possible Interaction with Tau

Cited by 176 publications

References 38 publications

Tau phosphorylation in Alzheimer's disease: pathogen or protector?

Tau phosphorylation in Alzheimer's disease: pathogen or protector?

Lipoic Acid and N-acetyl Cysteine Decrease Mitochondrial-Related Oxidative Stress in Alzheimer Disease Patient Fibroblasts

Involvement of PI3K/PKG/ERK1/2 signaling pathways in cortical neurons to trigger protection by cotreatment of acetyl-L-carnitine and α-lipoic acid against HNE-mediated oxidative stress and neurotoxicity: Implications for Alzheimer's disease

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