A Caenorhabditis elegans Parkin mutant with altered solubility couples {alpha}-synuclein aggregation to proteotoxic stress

doi:10.1093/hmg/ddi371

Human Molecular Genetics Advance Access published online on October 4, 2005
Human Molecular Genetics, doi:10.1093/hmg/ddi371

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© The Author 2005. Published by Oxford University Press. All rights reserved
Received June 7, 2005
Revised September 21, 2005
Accepted September 28, 2005

Article

A Caenorhabditis elegans Parkin mutant with altered solubility couples ${alpha}$ -synuclein aggregation to proteotoxic stress

Wolfdieter Springer ¹, Thorsten Hoppe ², Enrico Schmidt ³, and Ralf Baumeister ⁴^*

¹ ABI/Molecular Neurogenetics, University of Munich, Germany
² ABI/Molecular Neurogenetics, University of Munich, Germany; Centre for Molecular Neurobiology (ZMNH), University of Hamburg, Germany
³ Bio3/Bioinformatics & Molecular Genetics, University of Freiburg, Germany
⁴ ABI/Molecular Neurogenetics, University of Munich, Germany; Bio3/Bioinformatics & Molecular Genetics, University of Freiburg, Schaenzlestr. 1, 79104 Freiburg, Germany

^* To whom correspondence should be addressed.
Ralf Baumeister, E-mail: baumeister{at}celegans.de

Abstract

Mutations in the human parkin gene encoding an E3 ubiquitinligase have been associated with early-onset recessive formsof Parkinson’s disease (PD). However, the molecular mechanismsby which mutations in the parkin gene cause PD are still underdebate. Here, we identified and characterized the Caenorhabditiselegans parkin homolog, pdr-1. PDR-1 protein physically associatesand cooperates with a conserved degradation machinery to mediateubiquitin conjugation. Strikingly, in contrast to pdr-1 loss-of-functionmutants, an in-frame deletion variant with altered solubilityand intracellular localization properties is hypersensitivetowards different proteotoxic stress conditions. Both endoplasmicreticulum-derived folding stress and cytosolic stress conferredby expression of mutant human ${alpha}$ -synuclein resulted in severedevelopmental defects and lethality in pdr-1(lg103) mutant background.Furthermore, we show that the corresponding truncated proteinPDR-1( ${Delta}$ aa24-247) aggregates in cell culture, but still interactswith its ubiquitylation co-enzymes. Thus, it might block thecellular degradation/detoxification machinery and thereforerenders worms highly vulnerable to protein folding stress. Incontrast to other complete gene knock-outs or RNAi models ofParkin function, this C. elegans model recapitulates Parkininsolubility and aggregation similar to several AR-JP linkedParkin mutations. We suggest that such Parkin variants thateither confer a neomorphic function or a partial loss-of-functionmay help to further elucidate the biological function of Parkinin vivo and the pathogenic mechanisms resulting in AR-JP. Dueto high-throughput capacity of C. elegans, this model is particularlywell suited to identify genetic and chemical modifiers of toxicity.

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				J. Samann, J. Hegermann, E. von Gromoff, S. Eimer, R. Baumeister, and E. Schmidt Caenorhabditits elegans LRK-1 and PINK-1 Act Antagonistically in Stress Response and Neurite Outgrowth J. Biol. Chem., June 12, 2009; 284(24): 16482 - 16491. [Abstract] [Full Text] [PDF]

				R. Nass, K. M. Merchant, and T. Ryan Caenorhabditis elegans in Parkinson's Disease Drug Discovery: Addressing an Unmet Medical Need Mol. Interv., December 1, 2008; 8(6): 284 - 293. [Abstract] [Full Text] [PDF]

				M. C. K. Leung, P. L. Williams, A. Benedetto, C. Au, K. J. Helmcke, M. Aschner, and J. N. Meyer Caenorhabditis elegans: An Emerging Model in Biomedical and Environmental Toxicology Toxicol. Sci., November 1, 2008; 106(1): 5 - 28. [Abstract] [Full Text] [PDF]

				G. A. Caldwell and K. A. Caldwell Traversing a wormhole to combat Parkinson's disease Dis. Model. Mech., July 1, 2008; 1(1): 32 - 36. [Abstract] [Full Text] [PDF]

				K. Kawahara, M. Hashimoto, P. Bar-On, G. J. Ho, L. Crews, H. Mizuno, E. Rockenstein, S. Z. Imam, and E. Masliah {alpha}-Synuclein Aggregates Interfere with Parkin Solubility and Distribution: ROLE IN THE PATHOGENESIS OF PARKINSON DISEASE J. Biol. Chem., March 14, 2008; 283(11): 6979 - 6987. [Abstract] [Full Text] [PDF]

				R. Baumeister, E. Schaffitzel, and M. Hertweck Endocrine signaling in Caenorhabditis elegans controls stress response and longevity. J. Endocrinol., August 1, 2006; 190(2): 191 - 202. [Abstract] [Full Text] [PDF]

				Papers of Note Sci. Aging Knowl. Environ., October 12, 2005; 2005(41): nw38 - nw38. [Full Text]

Human Molecular Genetics

Article

A Caenorhabditis elegans Parkin mutant with altered solubility couples -synuclein aggregation to proteotoxic stress

A Caenorhabditis elegans Parkin mutant with altered solubility couples ${alpha}$ -synuclein aggregation to proteotoxic stress