Copper-binding-site-null SOD1 causes ALS in transgenic mice: aggregates of non-native SOD1 delineate a common feature

doi:10.1093/hmg/ddg312

. 2003 Nov 1;12(21):2753-64.

doi: 10.1093/hmg/ddg312. Epub 2003 Sep 9.

Copper-binding-site-null SOD1 causes ALS in transgenic mice: aggregates of non-native SOD1 delineate a common feature

Jiou Wang¹, Hilda Slunt, Victoria Gonzales, David Fromholt, Michael Coonfield, Neal G Copeland, Nancy A Jenkins, David R Borchelt

Affiliations

PMID: 12966034
DOI: 10.1093/hmg/ddg312

Copper-binding-site-null SOD1 causes ALS in transgenic mice: aggregates of non-native SOD1 delineate a common feature

Jiou Wang et al. Hum Mol Genet. 2003.

. 2003 Nov 1;12(21):2753-64.

doi: 10.1093/hmg/ddg312. Epub 2003 Sep 9.

Authors

Jiou Wang¹, Hilda Slunt, Victoria Gonzales, David Fromholt, Michael Coonfield, Neal G Copeland, Nancy A Jenkins, David R Borchelt

Affiliation

¹ Department of Pathology, The Johns Hopkins University School of Medicine, Baltimore, MD 21205, USA.

PMID: 12966034
DOI: 10.1093/hmg/ddg312

Abstract

Cu/Zn superoxide dismutase (SOD1), a crucial cellular antioxidant, can in certain settings mediate toxic chemistry through its Cu cofactor. Whether this latter property explains why mutations in SOD1 cause FALS has been debated. Here, we demonstrate motor neuron disease in transgenic mice expressing a SOD1 variant that mutates the four histidine residues that coordinately bind Cu. In-depth analyses of this new mouse model, previously characterized models and FALS human tissues revealed that the accumulation of detergent-insoluble forms of SOD1 is a common feature of the disease. These insoluble species include full-length SOD1 proteins, peptide fragments, stable oligomers and ubiquitinated entities. Moreover, chaperones Hsp25 and alphaB-crystallin specifically co-fractionated with insoluble SOD1. In cultured cells, all 11 of the FALS variants tested produced insoluble forms of mutant SOD1. Importantly, expression of recombinant peptide fragments of wild-type SOD1 in cultured cells also produced insoluble species, suggesting that SOD1 possesses elements with an intrinsic propensity to aggregate. Thus, modifications to the protein, such as FALS mutations, fragmentation and possibly covalent modification, may simply act to augment a natural, but potentially toxic, propensity to aggregate.

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Copper-binding-site-null SOD1 causes ALS in transgenic mice: aggregates of non-native SOD1 delineate a common feature

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Copper-binding-site-null SOD1 causes ALS in transgenic mice: aggregates of non-native SOD1 delineate a common feature

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