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TgCRND8小鼠在丰富饲养环境下淀粉样血管病和β淀粉样蛋白斑块负担减轻:多途径参与

Reduction of amyloid angiopathy and Abeta plaque burden after enriched housing in TgCRND8 mice: involvement of multiple pathways.

作者信息

Ambrée Oliver, Leimer Uwe, Herring Arne, Görtz Nicole, Sachser Norbert, Heneka Michael T, Paulus Werner, Keyvani Kathy

机构信息

University Hospital Münster, Institute of Neuropathology, Domagkstr. 19, D-48149, Münster, Germany.

出版信息

Am J Pathol. 2006 Aug;169(2):544-52. doi: 10.2353/ajpath.2006.051107.

Abstract

Diversity and intensity of intellectual and physical activities seem to have an inverse relationship with the extent of cognitive decline in Alzheimer's disease (AD). To study the interaction between an active lifestyle and AD pathology, female TgCRND8 mice carrying human APPswe+ind were transferred into enriched housing. Four months of continuous and diversified environmental stimulation resulted in a significant reduction of beta-amyloid (Abeta) plaques and in a lower extent of amyloid angiopathy. Neither human amyloid precursor protein (APP) mRNA/protein levels nor the level of carboxy-terminal fragments of APP nor soluble Abeta content differed between both groups, making alterations in APP expression or processing unlikely as a cause of reduced Abeta deposition. Moreover, DNA microarray analysis revealed simultaneous down-regulation of proinflammatory genes as well as up-regulation of molecules involved in anti-inflammatory processes, proteasomal degradation, and cholesterol binding, possibly explaining reduced Abeta burden by lower aggregation and enhanced clearance of Abeta. Additionally, immunoblotting against F4/80 antigen and morphometric analysis of microglia (Mac-3) revealed significantly elevated microgliosis in the enriched brains, which suggests increased amyloid phagocytosis. In summary, this study demonstrates that the environment interacts with AD pathology at dif-ferent levels.

摘要

智力和体力活动的多样性与强度似乎与阿尔茨海默病(AD)认知衰退的程度呈负相关。为了研究积极的生活方式与AD病理之间的相互作用,将携带人APPswe+ind的雌性TgCRND8小鼠转移到丰富环境饲养中。四个月持续且多样化的环境刺激导致β-淀粉样蛋白(Aβ)斑块显著减少,且淀粉样血管病程度降低。两组之间人淀粉样前体蛋白(APP)的mRNA/蛋白水平、APP羧基末端片段水平以及可溶性Aβ含量均无差异,这使得APP表达或加工的改变不太可能是Aβ沉积减少的原因。此外,DNA微阵列分析显示促炎基因同时下调,以及参与抗炎过程、蛋白酶体降解和胆固醇结合的分子上调,这可能通过降低Aβ聚集和增强Aβ清除来解释Aβ负担的减轻。此外,针对F4/80抗原的免疫印迹以及小胶质细胞(Mac-3)的形态计量分析显示,丰富环境饲养的大脑中小胶质细胞增生显著增加,这表明淀粉样蛋白吞噬作用增强。总之,本研究表明环境在不同水平上与AD病理相互作用。

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