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Severe Reactive Astrocytes Precipitate Pathological Hallmarks of Alzheimer’s Disease Via H2O2− Production

Journal of Autism and Developmental Disorders(2020)SCI 3区

Center for Cognition and Sociality | Center for Neuroscience | Department of Mechanical Engineering and Engineering Science | GNT Pharma Co. Ltd. | Virus Facility | Center for Glia-Neuron Interaction | Convergence Research Center for Diagnosis | Department of Biological Sciences | Genetics and Aging Research Unit | Precision Medicine Center | Integrated Science and Engineering Division | Neuroscience Program | School of Biological Sciences

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Abstract
Although the pathological contributions of reactive astrocytes have been implicated in Alzheimer’s disease (AD), their in vivo functions remain elusive due to the lack of appropriate experimental models and precise molecular mechanisms. Here, we show the importance of astrocytic reactivity on the pathogenesis of AD using GiD, a newly developed animal model of reactive astrocytes, where the reactivity of astrocytes can be manipulated as mild (GiDm) or severe (GiDs). Mechanistically, excessive hydrogen peroxide (H 2 O 2 ) originated from monoamine oxidase B in severe reactive astrocytes causes glial activation, tauopathy, neuronal death, brain atrophy, cognitive impairment and eventual death, which are significantly prevented by AAD-2004, a potent H 2 O 2 scavenger. These H 2 O 2 − -induced pathological features of AD in GiDs are consistently recapitulated in a three-dimensional culture AD model, virus-infected APP/PS1 mice and the brains of patients with AD. Our study identifies H 2 O 2 from severe but not mild reactive astrocytes as a key determinant of neurodegeneration in AD.
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Alzheimer's disease,Astrocyte,Biomedicine,general,Neurosciences,Behavioral Sciences,Biological Techniques,Neurobiology,Animal Genetics and Genomics
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要点】:本文揭示了重度反应性星形胶质细胞通过产生过氧化氢(H2O2)促进阿尔茨海默病(AD)的病理特征,并发现过氧化氢清除剂AAD-2004能显著预防这些病理变化。

方法】:研究使用GiD动物模型,该模型能够调控星形胶质细胞的反应性程度,分别为轻度(GiDm)和重度(GiDs),通过对比分析两种状态下星形胶质细胞的作用。

实验】:实验在GiD动物模型、三维培养的AD模型、APP/PS1小鼠以及阿尔茨海默病患者大脑中进行,结果表明重度反应性星形胶质细胞产生的过氧化氢是AD神经退行性的关键因素。