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来自野生型而非成年5xFAD小鼠的前脑小胶质细胞可防止器官型海马脑片培养物中淀粉样β斑块的形成。

Forebrain microglia from wild-type but not adult 5xFAD mice prevent amyloid-β plaque formation in organotypic hippocampal slice cultures.

作者信息

Hellwig Sabine, Masuch Annette, Nestel Sigrun, Katzmarski Natalie, Meyer-Luehmann Melanie, Biber Knut

机构信息

Department of Psychiatry and Psychotherapy, Freiburg, Germany.

Department of Neuroanatomy, Freiburg, Germany.

出版信息

Sci Rep. 2015 Sep 29;5:14624. doi: 10.1038/srep14624.

Abstract

The role of microglia in amyloid-β (Aβ) deposition is controversial. In the present study, an organotypic hippocampal slice culture (OHSC) system with an in vivo-like microglial-neuronal environment was used to investigate the potential contribution of microglia to Aβ plaque formation. We found that microglia ingested Aβ, thereby preventing plaque formation in OHSCs. Conversely, Aβ deposits formed rapidly in microglia-free wild-type slices. The capacity to prevent Aβ plaque formation was absent in forebrain microglia from young adult but not juvenile 5xFamilial Alzheimer's disease (FAD) mice. Since no loss of Aβ clearance capacity was observed in both wild-type and cerebellar microglia from 5xFAD animals, the high Aβ1-42 burden in the forebrain of 5xFAD animals likely underlies the exhaustion of microglial Aβ clearance capacity. These data may therefore explain why Aβ plaque formation has never been described in wild-type mice, and point to a beneficial role of microglia in AD pathology. We also describe a new method to study Aβ plaque formation in a cell culture setting.

摘要

小胶质细胞在β淀粉样蛋白(Aβ)沉积中的作用存在争议。在本研究中,我们使用具有类似体内小胶质细胞-神经元环境的器官型海马切片培养(OHSC)系统,来研究小胶质细胞对Aβ斑块形成的潜在作用。我们发现小胶质细胞摄取Aβ,从而防止OHSC中斑块的形成。相反,在无微胶质细胞的野生型切片中,Aβ沉积物迅速形成。成年但非幼年的5x家族性阿尔茨海默病(FAD)小鼠的前脑小胶质细胞缺乏防止Aβ斑块形成的能力。由于在5xFAD动物的野生型和小脑小胶质细胞中均未观察到Aβ清除能力的丧失,5xFAD动物前脑中高Aβ1-42负荷可能是小胶质细胞Aβ清除能力耗尽的基础。因此,这些数据可能解释了为什么在野生型小鼠中从未描述过Aβ斑块形成,并指出小胶质细胞在AD病理学中的有益作用。我们还描述了一种在细胞培养环境中研究Aβ斑块形成的新方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6af7/4586757/1e00842701e7/srep14624-f1.jpg

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