Mutation of SOD1 in ALS: a Gain of a Loss of Function

doi:10.1093/hmg/ddm110

Human Molecular Genetics Advance Access published online on May 15, 2007
Human Molecular Genetics, doi:10.1093/hmg/ddm110

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Mutation of SOD1 in ALS: a Gain of a Loss of Function

Daniela Sau¹^,5, Silvia De Biasi², Laura Vitellaro-Zuccarello², Patrizia Riso³, Serena Guarnieri³, Marisa Porrini³, Silvia Simeoni¹, Valeria Crippa¹^,5, Elisa Onesto¹^,5, Isabella Palazzolo¹^,5, Paola Rusmini¹^,5, Elena Bolzoni¹^,5, Caterina Bendotti⁴ and Angelo Poletti¹^,5^,*

¹ Institute of Endocrinology, Center of Excellence on Neurodegenerative Diseases of the University of Milan ( Italy) ² Department of Biomolecular Sciences and Biotechnologies, University of Milan ( Italy) ³ Department of Food Science-and Microbiology, Division of Human Nutrition, University of Milan ( Italy) ⁴ Department of Neuroscience, Istituto di Ricerche Farmacologiche Mario Negri, Milan ( Italy) ⁵ InterUniversity Center on Neurodegenerative Diseases of the Universities of Florence, Rome and Milan ( Italy)

^* Corresponding Author: Angelo Poletti, Institute of Endocrinology- Center of Excellence on Neurodegenerative Diseases University of Milan- Via Balzaretti 9, 20133 Milano ( Italy), Ph +39-02-5031.8215, Fax +39-02-5031.8204, e-mail: angelo.poletti{at}unimi.it

Received October 6, 2006; Revised April 25, 2007; Accepted April 25, 2007

Amyotrophic lateral sclerosis is a neurodegenerative diseasecaused by motoneuron loss. Some familial cases (fALS) are linkedto mutations of Superoxide-Dismutase type-1 (SOD1), an antioxidantenzyme whose activity is preserved in most mutant forms. Dueto the similarities in sporadic and fALS forms, mutant SOD1animal and cellular models are a useful tool to study the disease.In transgenic mice expressing either wild type (wt) human SOD1or mutant G93A-SOD1, we found that wtSOD1 was present in cytoplasmand in nuclei of motoneurons, while mutant SOD1 was mainly cytoplasmic.Similar results were obtained in immortalized motoneurons (NSC34cells) expressing either wt or G93A-SOD1. Analysing the proteasomeactivity, responsible for misfolded protein clearance, in thetwo subcellular compartments we found proteasome impairmentonly in the cytoplasm. The effect of G93A-SOD1 exclusion fromnuclei was then analyzed after oxidative stress. Cells expressingG93A-SOD1 showed a higher DNA damage compared to those expressingwtSOD1, possibly because of a loss of nuclear protection. Thetoxicity of mutant SOD1 might therefore arise from an initialmisfolding (gain-of-function) reducing nuclear protection fromthe active enzyme (loss-of-function in the nuclei), a processthat may be involved in ALS pathogenesis.

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