Author:
Sangwan Smriti,Zhao Anni,Adams Katrina L.,Jayson Christina K.,Sawaya Michael R.,Guenther Elizabeth L.,Pan Albert C.,Ngo Jennifer,Moore Destaye M.,Soriaga Angela B.,Do Thanh D.,Goldschmidt Lukasz,Nelson Rebecca,Bowers Michael T.,Koehler Carla M.,Shaw David E.,Novitch Bennett G.,Eisenberg David S.
Abstract
Fibrils and oligomers are the aggregated protein agents of neuronal dysfunction in ALS diseases. Whereas we now know much about fibril architecture, atomic structures of disease-related oligomers have eluded determination. Here, we determine the corkscrew-like structure of a cytotoxic segment of superoxide dismutase 1 (SOD1) in its oligomeric state. Mutations that prevent formation of this structure eliminate cytotoxicity of the segment in isolation as well as cytotoxicity of the ALS-linked mutants of SOD1 in primary motor neurons and in a Danio rerio (zebrafish) model of ALS. Cytotoxicity assays suggest that toxicity is a property of soluble oligomers, and not large insoluble aggregates. Our work adds to evidence that the toxic oligomeric entities in protein aggregation diseases contain antiparallel, out-of-register β-sheet structures and identifies a target for structure-based therapeutics in ALS.
Funder
Howard Hughes Medical Institute
HHS | National Institutes of Health
Publisher
Proceedings of the National Academy of Sciences
Cited by
98 articles.
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