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Unique pathological tau conformers from Alzheimer’s brains transmit tau pathology in nontransgenic mice

机译:来自阿尔茨海默氏症大脑的独特病理tau构象异构体在非转基因小鼠中传播tau病理

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摘要

Filamentous tau aggregates are hallmark lesions in numerous neurodegenerative diseases, including Alzheimer’s disease (AD). Cell culture and animal studies showed that tau fibrils can undergo cell-to-cell transmission and seed aggregation of soluble tau, but this phenomenon was only robustly demonstrated in models overexpressing tau. In this study, we found that intracerebral inoculation of tau fibrils purified from AD brains (AD-tau), but not synthetic tau fibrils, resulted in the formation of abundant tau inclusions in anatomically connected brain regions in nontransgenic mice. Recombinant human tau seeded by AD-tau revealed unique conformational features that are distinct from synthetic tau fibrils, which could underlie the differential potency in seeding physiological levels of tau to aggregate. Therefore, our study establishes a mouse model of sporadic tauopathies and points to important differences between tau fibrils that are generated artificially and authentic ones that develop in AD brains.
机译:丝状tau聚集体是许多神经退行性疾病(包括阿尔茨海默氏病(AD))的标志性病变。细胞培养和动物研究表明,tau原纤维可以进行细胞间传递和可溶性tau的种子聚集,但是这种现象仅在过表达tau的模型中得到有力证明。在这项研究中,我们发现从AD大脑(AD-tau)纯化的tau原纤维的脑内接种,而不是合成的tau原纤维,在非转基因小鼠的解剖学上相连的大脑区域中形成大量tau内含物。用AD-tau接种的重组人tau揭示了独特的构象特征,这些特征不同于合成的tau原纤维,这可能是在播种tau的生理水平聚集时可能具有的不同能力。因此,我们的研究建立了散发性tauopathies的小鼠模型,并指出了人工产生的tau纤维与在AD脑中发育的真实tau纤维之间的重要差异。

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