Minimally Toxic Dose of Lipopolysaccharide and α-Synuclein Oligomer Elicit Synergistic Dopaminergic Neurodegeneration: Role and Mechanism of Microglial NOX2 Activation

被引:0
|
作者
Wei Zhang
Jun-hua Gao
Zhao-fen Yan
Xi-yan Huang
Peng Guo
Li Sun
Zhuo Liu
Yang Hu
Li-jun Zuo
Shu-yang Yu
Chen-Jie Cao
Xiao-min Wang
Jau-shyong Hong
机构
[1] Capital Medical University,Department of Geriatrics, Beijing Tiantan Hospital
[2] Beijing Tiantian Hospital,Department of Neurology
[3] Capital Medical University,Center of Parkinson’s Disease
[4] China National Clinical Research Center for Neurological Diseases,Departments of Neurobiology and Physiology
[5] Key Laboratory for Neurodegenerative Disorders of the Ministry of Education,Neuropharmacology Section, Laboratory of Pharmacology and Chemistry
[6] Beijing Institute for Brain Disorders,undefined
[7] Beijing Key Laboratory on Parkinson’s Disease,undefined
[8] Capital Medical University,undefined
[9] National Institute of Environmental Health Sciences/National Institutes of Health,undefined
来源
Molecular Neurobiology | 2018年 / 55卷
关键词
Parkinson disease; Environmental factors; Lipopolysaccharide; α-Synuclein oligomer; Synergistic; Dopaminergic neurodegeneration; Microglial activation;
D O I
暂无
中图分类号
学科分类号
摘要
The aim of this study is to investigate the role and mechanism of microglial NOX2 activation in minimally toxic dose of LPS and Syn-elicited synergistic dopaminergic neurodegeneration. NOX2+/+ and NOX2−/− mice and multiple primary cultures were treated with LPS and/or Syn in vivo and in vitro. Neuronal function and morphology were evaluated by uptake of related neurotransmitter and immunostaining with specific antibody. Levels of superoxide, intracellular reactive oxygen species, mRNA and protein of relevant molecules, and dopamine were detected. LPS and Syn synergistically induce selective and progressive dopaminergic neurodegeneration. Microglia are functionally and morphologically activated, contributing to synergistic dopaminergic neurotoxicity elicited by LPS and Syn. NOX2−/− mice are more resistant to synergistic neurotoxicity than NOX2+/+mice in vivo and in vitro, and NOX2 inhibitor protects against synergistic neurotoxicity through decreasing microglial superoxide production, illustrating a critical role of microglial NOX2. Microglial NOX2 is activated by LPS and Syn as mRNA and protein levels of NOX2 subunits P47and gp91 are enhanced. Molecules relevant to microglial NOX2 activation include PKC-σ, P38, ERK1/2, JNK, and NF-КBP50 as their mRNA and protein levels are elevated after treatment with LPS and Syn. Combination of exogenous and endogenous environmental factors with minimally toxic dose synergistically propagates dopaminergic neurodegeneration through activating microglial NOX2 and relevant signaling molecules, casting a new light for PD pathogenesis.
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页码:619 / 632
页数:13
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