Olanzapine protects PC12 cells from oxidative stress induced by hydrogen peroxide

被引：123

作者：

Wei, ZL

Bai, O

Richardson, JS

Mousseau, DD

Li, XM

机构：

[1] Univ Saskatchewan, Neuropsychiat Res Unit, Coll Med, Dept Psychiat, Saskatoon, SK S7N 5E3, Canada

[2] Univ Saskatchewan, Coll Med, Dept Pharmacol, Saskatoon, SK S7N 0W0, Canada

来源：

JOURNAL OF NEUROSCIENCE RESEARCH | 2003年 / 73卷 / 03期

关键词：

SOD-1; neuroleptics; hydrogen peroxide; neuroprotection;

D O I：

10.1002/jnr.10668

中图分类号：

Q189 [神经科学];

学科分类号：

071006 ;

摘要：

Neuroanatomical studies suggest that neuronal atrophy and destruction occur over the course of many years in neurodegenerative conditions such as schizophrenia and Alzheimer's disease. In schizophrenia, early intervention with atypical neuroleptics such as olanzapine has been shown to prevent development of some of the more serious and debilitating symptoms in many patients. The mechanisms whereby olanzapine slows or prevents symptom progression in schizophrenia remain unclear. A previous study found that olanzapine increased mRNA for the copper/zinc isoform of the superoxide dismutase enzyme (SOD-1). We investigated the effects of olanzapine in PC12 cells exposed to hydrogen peroxide. We measured cell viability, observed evidence of necrosis and apoptosis, checked the SOD-1 mRNA by Northern blot analyses, and determined SOD-1 enzyme activity. We found that: 1) the decrease in cell viability induced by hydrogen peroxide was attenuated in PC12 cells pre-treated with olanzapine; 2) olanzapine increased SOD enzyme activity in PC12 cells; 3) inhibiting SOD activity with diethyldithiocarbamic acid prevented the cytoprotective actions of olanzapine; and 4) the decrease in SOD-1 mRNA level induced by hydrogen peroxide was blocked by pretreatment with olanzapine. These data indicate that the neuroprotective action of olanzapine includes the upregulation of SOD. (C) 2003 Wiley-Liss, Inc.

引用

页码：364 / 368

页数：5

共 32 条

[11]

Li XM, 1999, J NEUROSCI RES, V56, P72, DOI 10.1002/(SICI)1097-4547(19990401)56:1<72::AID-JNR9>3.0.CO

[12]

2-0

[13] Oxidative stress hypothesis in Alzheimer's disease [J].

Markesbery, WR .

FREE RADICAL BIOLOGY AND MEDICINE, 1997, 23 (01) :134-147

[14]

Maroto R, 1997, J NEUROCHEM, V69, P514

[15] RAPID COLORIMETRIC ASSAY FOR CELLULAR GROWTH AND SURVIVAL - APPLICATION TO PROLIFERATION AND CYTO-TOXICITY ASSAYS [J].

MOSMANN, T .

JOURNAL OF IMMUNOLOGICAL METHODS, 1983, 65 (1-2) :55-63

[16]

Pappolla MA, 1997, J NEUROSCI, V17, P1683

[17] Inhibition of neuronal apoptosis by a metalloporphyrin superoxide dismutase mimic [J].

Patel, M .

JOURNAL OF NEUROCHEMISTRY, 1998, 71 (03) :1068-1074

[18] FREE-RADICALS IN THE GENESIS OF ALZHEIMERS-DISEASE [J].

RICHARDSON, JS .

ALZHEIMERS DISEASE: AMYLOID PRECUSOR PROTEINS, SIGNAL TRANSDUCTION, AND NEURONAL TRANSPLANTATION, 1993, 695 :73-76

[19] ON THE POSSIBLE ROLE OF IRON-INDUCED FREE-RADICAL PEROXIDATION IN NEURAL DEGENERATION IN ALZHEIMERS-DISEASE [J].

RICHARDSON, JS ;

SUBBARAO, KV ;

ANG, LC .

ANNALS OF THE NEW YORK ACADEMY OF SCIENCES, 1992, 648 :326-327

[20] CHRONIC INHIBITION OF SUPEROXIDE-DISMUTASE PRODUCES APOPTOTIC DEATH OF SPINAL NEURONS [J].

ROTHSTEIN, JD ;

BRISTOL, LA ;

HOSLER, B ;

BROWN, RH ;

KUNCL, RW .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1994, 91 (10) :4155-4159

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