期刊
NATURE COMMUNICATIONS
卷 8, 期 -, 页码 -出版社
NATURE PUBLISHING GROUP
DOI: 10.1038/s41467-017-02056-4
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资金
- KID PhD studentship grant (FRK)
- Swedish Research Council
- Center for Innovative Medicine (CIMED)
- Swedish Alzheimer foundation
- Swedish Brain Foundation
- Karolinska Institutet
- Stiftelsen fur Gamla Tjanarinnor
- Instruct RD pilot project [APPID 272]
- Loo and Hans Osterman Foundation
- Geriatric Diseases Foundation at Karolinska Institutet
- VIAA Latvia [NFI/R/2014/023]
- Latvian Institute of Organic Synthesis
. Protein misfolding and aggregation is increasingly being recognized as a cause of disease. In Alzheimer's disease the amyloid-beta peptide (A beta) misfolds into neurotoxic oligomers and assembles into amyloid fibrils. The Bri2 protein associated with Familial British and Danish dementias contains a BRICHOS domain, which reduces A beta fibrillization as well as neurotoxicity in vitro and in a Drosophila model, but also rescues proteins from irreversible nonfibrillar aggregation. How these different activities are mediated is not known. Here we show that Bri2 BRICHOS monomers potently prevent neuronal network toxicity of A beta, while dimers strongly suppress A beta fibril formation. The dimers assemble into high-molecular-weight oligomers with an apparent two-fold symmetry, which are efficient inhibitors of non-fibrillar protein aggregation. These results indicate that Bri2 BRICHOS affects qualitatively different aspects of protein misfolding and toxicity via different quaternary structures, suggesting a means to generate molecular chaperone diversity.
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