Increased AP-1 DNA-Binding Activity and Nuclear REF-1 Accumulation in Lead-Exposed Primary Cultures of Astrocytes

被引:0
|
作者
Marzia Scortegagna
Ingeborg Hanbauer
机构
[1] NHLBI,Laboratory of Molecular Immunology
[2] NIH,Laboratory of Molecular Immunology
[3] NHLBI,undefined
[4] NIH,undefined
来源
Neurochemical Research | 2000年 / 25卷
关键词
Activator protein-1; c-jun mRNA; redox factor-1 protein; lead; astrocyte primary cultures;
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学科分类号
摘要
Pb was shown to perturb neuronal and glial function either directly by interacting with protein thiol groups or indirectly by mimicking Ca2+ and increasing oxidative stress. In view of the potential action of Pb on cellular redox homeostasis we studied the regulation of activator protein-1 (AP-1) DNA binding. A 1h incubation of astrocyte primary cultures with 10 μM Pb caused a 2.5 fold increase in AP-1 DNA binding. An assessment of how Pb elicited this increase revealed the involvement of 1. transcriptional and 2. posttranslational processes. The first one was documented by an increase of c-jun mRNA content after 15 to 30 min of 10 μM Pb exposure. The second one was suggested by an enhanced nuclear accumulation of redox factor-1 after 30 to 60 min of 10 μM Pb exposure. The Pb-elicited increase of the reduction/oxidation-sensitive AP-1 signal transduction may regulate target genes operative in cell survival or cell death.
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页码:861 / 866
页数:5
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