期刊
METHODS
卷 53, 期 3, 页码 295-305出版社
ACADEMIC PRESS INC ELSEVIER SCIENCE
DOI: 10.1016/j.ymeth.2010.12.008
关键词
Amyloid; Plate reader assay; Thioflavin T; Shared micelles; SDS; Trifluoroethanol; Natively disordered proteins; Alpha-synuclein
资金
- Danish Ministry of Science, Technology and Innovation
- Michael J. Fox Foundation for Parkinson's Research
This review describes different ways to achieve and monitor reproducible aggregation of alpha-synuclein, a key protein in the development of Parkinson's disease. For most globular proteins, aggregation is promoted by partially denaturing conditions which compromise the native state without destabilizing the intermolecular contacts required for accumulation of regular amyloid structure. As a natively disordered protein, alpha-synuclein can fibrillate under physiological conditions and this process is actually stimulated by conditions that promote structure formation, such as low pH, ions, polyamines, anionic surfactants, fluorinated alcohols and agitation. Reproducibility is a critical issue since alpha-synuclein shows erratic fibrillation behavior on its own. Agitation in combination with glass beads significantly reduces the variability of aggregation time curves, but the most reproducible aggregation is achieved by sub-micellar concentrations of SDS, which promote the rapid formation of small clusters of alpha-synuclein around shared micelles. Although the fibrils produced this way have a different appearance and secondary structure, they are rich in cross-beta structure and are amenable to high-throughput screening assays. Although such assays at best provide a very simplistic recapitulation of physiological conditions, they allow the investigator to focus on well-defined molecular events and may provide the opportunity to identify, e.g. small molecule inhibitors of aggregation that affect these steps. Subsequent experiments in more complex cellular and whole-organism environments can then validate whether there is any relation between these molecular interactions and the broader biological context. (C) 2010 Elsevier Inc. All rights reserved.
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