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Article
Dithiol-based compounds maintain expression of antioxidant protein peroxiredoxin 1 that counteracts toxicity of mutant huntingtin
Journal of Biological Chemistry
  • Andrea Pitts, Western University
  • Kyle Dailey, Western University
  • Jordan T. Newington, Western University
  • Andrew Chien, Western University
  • Robert Arseneault, Western University
  • Tyler Cann, Western University
  • Leslie M. Thompson, UCI School of Medicine
  • Robert C. Cumming, Western University
Document Type
Article
Publication Date
6-29-2012
URL with Digital Object Identifier
10.1074/jbc.M111.334565
Abstract

Mitochondrial dysfunction and elevated reactive oxygen species are strongly implicated in both aging and various neurodegenerative disorders, including Huntington disease (HD). Because reactive oxygen species can promote the selective oxidation of protein cysteine sulfhydryl groups to disulfide bonds we examined the spectrum of disulfide-bonded proteins that were specifically altered in a HD context. Protein extracts from PC12 cells overexpressing the amino-terminal fragment of the Huntingtin (Htt) protein with either a nonpathogenic or pathogenic polyglutamine repeat (Htt-103Q) were resolved by redox two-dimensional PAGE followed by mass spectrometry analysis. Several antioxidant proteins were identified that exhibited changes in disulfide bonding unique to Htt-103Q expressing cells. In particular, the antioxidant protein peroxiredoxin 1 (Prx1) exhibited both decreased expression and hyperoxidation in response to mutant Htt expressed in either PC12 cells or immortalized striatal cells exposed to 3-nitropropionic acid. Ectopic expression of Prx1 in PC12 cells attenuated mutant Httinduced toxicity. In contrast, short hairpin RNA-mediated knockdown of Prx1 potentiated mHtt toxicity. Furthermore, treatment with the dithiol-based compounds dimercaptopropanol and dimercaptosuccinic acid suppressed toxicity in bothHD cell models, whereas monothiol compounds were relatively ineffective. Dimercaptopropanol treatment also prevented mutant Htt-induced loss of Prx1 expression in both cell models. Our studies reveal for the first time that pathogenic Htt can affect the expression and redox state of antioxidant proteins; an event countered by specific dithiol-based compounds. These findings should provide a catalyst to explore the use of dithiolbased drugs for the treatment of neurodegenerative diseases. © 2012 by The American Society for Biochemistry and Molecular Biology, Inc.

Citation Information
Andrea Pitts, Kyle Dailey, Jordan T. Newington, Andrew Chien, et al.. "Dithiol-based compounds maintain expression of antioxidant protein peroxiredoxin 1 that counteracts toxicity of mutant huntingtin" Journal of Biological Chemistry Vol. 287 Iss. 27 (2012) p. 22717 - 22729
Available at: http://works.bepress.com/robert-cumming/5/