Impaired Extracellular Secretion of Mutant Superoxide Dismutase 1 Associates with Neurotoxicity in Familial Amyotrophic Lateral Sclerosis

doi:10.1523/JNEUROSCI.4253-04.2005

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The Journal of Neuroscience, January 5, 2005, 25(1):108-117; doi:10.1523/JNEUROSCI.4253-04.2005

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Neurobiology of Disease
Impaired Extracellular Secretion of Mutant Superoxide Dismutase 1 Associates with Neurotoxicity in Familial Amyotrophic Lateral Sclerosis
Bradley J. Turner,¹^,2 Julie D. Atkin,¹ Manal A. Farg,¹ Da Wei Zang,¹ Alan Rembach,¹ Elizabeth C. Lopes,¹ Justin D. Patch,¹ Andrew F. Hill,²^,3 and Surindar S. Cheema¹
¹Howard Florey Institute of Experimental Physiology and Medicine and Departments of ²Biochemistry and Molecular Biology and ³Pathology, University of Melbourne, Victoria 3010, Australia

Mutations in the intracellular metalloenzyme superoxide dismutase1 (SOD1) are linked to neurotoxicity in familial amyotrophiclateral sclerosis (ALS) by an unclear mechanism. Golgi fragmentationand endoplasmic reticulum stress are early hallmarks of spinalmotor neuron pathology in transgenic mice overexpressing mutantSOD1, suggesting that dysfunction of the neuronal secretorypathway may contribute to ALS pathogenesis. We therefore proposedthat mutant SOD1 directly engages and modulates the secretorypathway based on recent evidence of SOD1 secretion in diversehuman cell lines. Here, we demonstrate that a fraction of activeendogenous SOD1 is secreted by NSC-34 motor neuron-like cellsvia a brefeldin-A (BFA)-sensitive pathway. Expression of enhancedgreen fluorescent protein-tagged mutant human SOD1 (hSOD1-EGFP)in NSC-34 cells induced frequent cytoplasmic inclusions andprotein insolubility that correlated with toxicity. In contrast,transfection of non-neuronal COS-7 cells resulted in mutanthSOD1-EGFP cytoplasmic inclusions, oligomerization, and fragmentationwithout detectable toxicity. Importantly, impaired secretionof hSOD1-EGFP was common to all 10 SOD1 mutants tested relativeto wild-type protein in NSC-34 cells. Treatment with BFA inhibitedhSOD1-EGFP secretion with pronounced BFA-induced toxicity inmutant cells. Extracellular targeting of mutant hSOD1-EGFP viaSOD3 signal peptide fusion attenuated cytoplasmic inclusionformation and toxicity. The effect of elevated extracellularSOD1 was then evaluated in a transgenic rat model of ALS. Chronicintraspinal infusion of exogenous wild-type hSOD1 significantlydelayed disease progression and endpoint in transgenic SOD1^G93Arats. Collectively, these results suggest novel extracellularroles for SOD1 in ALS and support a causal relationship betweenmutant SOD1 secretion and intraneuronal toxicity.

Key words: amyotrophic lateral sclerosis; CSF; neuronal inclusion; NSC-34 cell; protein aggregation; secretion; superoxide dismutase 1; transgenic rat

Received Oct 13, 2004; revised November 11, 2004; accepted November 11, 2004.

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