Journal
PLOS ONE
Volume 6, Issue 1, Pages -Publisher
PUBLIC LIBRARY SCIENCE
DOI: 10.1371/journal.pone.0016706
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Funding
- Morris K. Udall Parkinson's Disease Research Center
- National Institutes of Health-National Institute of Neurological Disorders and Stroke [NS 38377, NS 38065]
- NIH [NS06885, NS062165]
- US Public Health Service [K08-NS020235]
- Parkinson Disease Foundation
- American Parkinson Disease Association
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Genetic and biochemical abnormalities of alpha-synuclein are associated with the pathogenesis of Parkinson's disease. In the present study we investigated the in vivo interaction of mouse and human alpha-synuclein with the potent parkinsonian neurotoxin, MPTP. We find that while lack of mouse alpha-synuclein in mice is associated with reduced vulnerability to MPTP, increased levels of human alpha-synuclein expression is not associated with obvious changes in the vulnerability of dopaminergic neurons to MPTP. However, expressing human alpha-synuclein variants (human wild type or A53T) in the alpha-synuclein null mice completely restores the vulnerability of nigral dopaminergic neurons to MPTP. These results indicate that human alpha-synuclein can functionally replace mouse alpha-synuclein in regard to vulnerability of dopaminergic neurons to MPTP-toxicity. Significantly, alpha-synuclein null mice and wild type mice were equally sensitive to neurodegeneration induced by 2'NH2-MPTP, a MPTP analog that is selective for serotoninergic and noradrenergic neurons. These results suggest that effects of alpha-synuclein on MPTP like compounds are selective for nigral dopaminergic neurons. Immunoblot analysis of beta-synuclein and Akt levels in the mice reveals selective increases in beta-synuclein and phosphorylated Akt levels in ventral midbrain, but not in other brain regions, of alpha-synuclein null mice, implicating the a-synuclein-level dependent regulation of beta-synuclein expression in modulation of MPTP-toxicity by alpha-synuclein. Together these findings provide new mechanistic insights on the role alpha-synuclein in modulating neurodegenerative phenotypes by regulation of Akt-mediated cell survival signaling in vivo.
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