Small stress molecules inhibit aggregation and neurotoxicity of prion peptide 106-126
In prion diseases, the posttranslational modification of host-encoded prion protein PrPc yields a high beta-sheet content modified protein PrPsc, which further polymerizes into amyloid fibrils. PrP106-126 initiates the conformational changes leading to the conversion of PrPc to PrPsc. Molecules that can defunctionalize such peptides can serve as a potential tool in combating prion diseases. In microorganisms during stressed conditions, small stress molecules (SSMs) are formed to prevent protein denaturation and maintain protein stability and function. The effect of such SSMs on PrP106-126 amyloid formation is explored in the present study using turbidity, atomic force microscopy (AFM), and cellular toxicity assay. Turbidity and AFM studies clearly depict that the SSMs-ectoine and mannosylglyceramide (MGA) inhibit the PrP106-126 aggregation. Our study also connotes that ectoine and MGA offer strong resistance to prion peptide-induced toxicity in human neuroblastoma cells, concluding that such molecules can be potential inhibitors of prion aggregation and toxicity. (C) 2007 Elsevier Inc. All rights reserved.
- Publisher
- Academic Press Inc Elsevier Science
- Issue Date
- 2008-01
- Language
- English
- Article Type
- Article
- Keywords
COMPATIBLE SOLUTES; PROTEIN-FRAGMENT; LACTATE-DEHYDROGENASE; RHODOTHERMUS-MARINUS; FIBRIL FORMATION; MANNOSYLGLYCERATE; RESIDUES-106-126; HYDROXYECTOINE; STABILIZATION; ACCUMULATION
- Citation
BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, v.365, no.4, pp.808 - 813
- ISSN
- 0006-291X
- Appears in Collection
- MS-Journal Papers(저널논문)
- Files in This Item
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