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Novel model of secreted human tau protein reveals the impact of the abnormal N-glycosylation of tau on its aggregation propensity.

Sci Rep. 2019; 
LosevYelena,PaulAshim,Frenkel-PinterMoran,Abu-HusseinMalak,KhalailaIsam,GazitEhud,SegalDa
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Catalog Antibody … Thank you for visiting nature.com. You are using a browser version with limited support for CSS … To that end, the transfected cells were immunostained using both 5A6, an antibody detecting total tau, and sc-11397, recognizing calnexin, an ER membrane bound chaperon 23 …polyacrylamide gels (GenScript) using a Mini-PROTEAN Tetra Vertical Electrophoresis Cell apparatus (Bio-Rad) Get A Quote

摘要

Alzheimer's disease (AD) is the most common neurodegenerative disorder and has no disease-modifying treatment yet. The hallmarks of AD are two amyloidogenic proteins: tau and amyloid β (Aβ). Tau undergoes several posttranslational modifications, including N-glycosylation. Tau was reported to be N-glycosylated in AD brains, but not in healthy counterparts, which may affect AD etiology. Here, we aimed to examine the effect of N-glycosylation on aggregation propensity of tau. To that end, a novel SH-SY5Y cell-based model was generated in which recombinant human tau (htau) is forced to be secreted from the cells. Secreted htau was found to localize in the secretory pathway compartments and to undergo N-... More

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