アルツハイマー病とレビー小体型認知症の複合病態で神経細胞死が進行する~モデルマウスを用いた解析による研究成果~

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2025-08-01 早稲田大学

早稲田大学などの研究グループは、アルツハイマー病とレビー小体型認知症の複合病態を再現したダブルトランスジェニックマウスを用い、単独疾患モデルと比較解析を行いました。タウとα-シヌクレインを過剰発現させたこのモデルでは、8か月齢でタウのリン酸化や神経炎症、海馬CA1の神経細胞死が著しく進行し、記憶障害も顕著に現れました。この結果は、両疾患が併発すると病態進行が加速する可能性を示唆しています。研究はMolecular Neurobiology誌に掲載。

アルツハイマー病とレビー小体型認知症の複合病態で神経細胞死が進行する~モデルマウスを用いた解析による研究成果~図1  海馬CA1領域の神経細胞数の比較

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神経細胞における変異型タウとα-シヌクレインの共発現は、マウス脳におけるタウのリン酸化、神経細胞の喪失、および神経炎症を促進する Co-Expression of Mutant Tau and α-Synuclein in Neurons Promotes Tau Phosphorylation, Neuronal Loss, and Neuroinflammation in Mouse Brain

Yuki Yamamoto,Toshiki Kubota,Daisuke Noguchi,Takaomi C. Saido & Toshio Ohshima
Molecular Neurobiology  Published:25 July 2025
DOI:https://doi.org/10.1007/s12035-025-05248-y

Abstract

Intracellular aggregation and accumulation of protein is a hallmark of neurodegenerative diseases. Tauopathy, which is caused by aggregated tau accumulation, is a group of neurodegenerative diseases, including frontotemporal dementia (FTD), Pick disease, and Alzheimer’s disease. Similarly, synucleinopathy, which is caused by aggregated α-synuclein (α-syn) accumulation, includes Parkinson’s disease and dementia with Lewy body (DLB). The interaction between tau and α-syn has been attracting attention because of similarities in symptoms and the co-existence of tau and α-syn in neural cells. Previous studies revealed that tau and α-syn promote their aggregation with each other. Additionally, other studies showed that α-syn promotes tau spreading in the mouse brain. In the present study, we investigated the relationship between tau and α-syn and the effects of their co-existence in neuronal cells on mouse pathology by double transgenic strategy. Consequently, we found increased phosphorylated tau, a declined number of neurons in the CA1 region, and increased astrocyte and microglia in the hippocampi in double transgenic mice at 8 months old. In mice that co-express tau and α-syn, locomotive activity increased and cognitive function decreased in behavioral test. These results suggest the co-existence of tau andα-syn in neurons that promote neuronal loss and impaired cognitive function in neurodegenerative conditions.

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