| Literature DB >> 24919397 |
Md Mamunul Haque1, Dohee Kim, Young Hyun Yu, Sungsu Lim, Dong Jin Kim, Young-Tae Chang, Hyung-Ho Ha, Yun Kyung Kim.
Abstract
Abnormal tau aggregates are presumed to be neurotoxic and are an important therapeutic target for multiple neurodegenerative disorders including Alzheimer's disease. Growing evidence has shown that tau intermolecular disulfide cross-linking is critical in generating tau oligomers that serve as a building block for higher-order aggregates. Here we report that a small molecule inhibitor prevents tau aggregation by blocking the generation of disulfide cross-linked tau oligomers. Among the compounds tested, a rosamine derivative bearing mild thiol reactivity selectively labeled tau and effectively inhibited oligomerization and fibrillization processes in vitro. Our data suggest that controlling tau oxidation status could be a new therapeutic strategy for prevention of abnormal tau aggregation.Entities:
Keywords: In-gel fluorescence; Tau oligomerization; intermolecular disulfide bond; rosamine; small molecule inhibitor; thiol reactivity
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Year: 2014 PMID: 24919397 DOI: 10.3109/13506129.2014.929103
Source DB: PubMed Journal: Amyloid ISSN: 1350-6129 Impact factor: 7.141