This proposal is for molecular genetic assessment of SNCA in alpha-synucleinopathy. Our data
shows alpha-synuclein overexpression is sufficient to give rise to a spectrum of Parkinsonism
disorders, including Parkinson's disease, parkinsonism and dementia, dementia with Lewy
bodies and multiple system atrophy; alpha-synuclein is undoubtedly a central component in
sporadic and familial disease.
Our aims are to: 1) identify genetic variability in the SNCA locus and determine what
contribution it has to these phenotypes; 2) molecularly, clinically and pathologically
characterize SNCA multiplication mutations;, 3) quantify SNCA gene expression in normal
aging and disease, and; 4) functionally assess genetic variability within the gene and its
promoter. Furthermore, we are to examine the transcriptional consequence of alpha-synuclein
over-expression, in model systems, in human brain tissue from cases with SNCA
multiplication.
Our objective is to provide meaningful molecular diagnoses to reclassify this heterogeneous
group of diseases, into distinct groups, for further longitudinal and pathological assessment.
As alpha-synuclein has an extended half-life (approximately 30hrs), thus our work is focused on characterizing SNCA genetic variability, transcriptional regulation and mRNA expression. We posit reduction in alpha-synuclein expression may provide a powerful therapeutic strategy to prevent alpha-synucleinopathy or halt its progression.
National Institute of Neurological Disorders and Stroke
CFDA Code
DUNS Number
153223151
UEI
GKPBCFV1QMM3
Project Start Date
01-July-2004
Project End Date
31-August-2009
Budget Start Date
01-July-2004
Budget End Date
31-August-2005
Project Funding Information for 2004
Total Funding
$256,003
Direct Costs
$170,669
Indirect Costs
$85,334
Year
Funding IC
FY Total Cost by IC
2004
National Institute of Neurological Disorders and Stroke
$256,003
Year
Funding IC
FY Total Cost by IC
Sub Projects
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