Abstract

The hypothesis driving this proposal is that presynaptic dysfunction is a common causative factor leading to cell death in multiple inherited neurodegenerative diseases. This hypothesis is based on the observations that 1) synaptic function mediates neuronal survival during development, 2) mutations which strongly impair presynaptic function result in massive, progressive neuronal degeneration, 3) a number of presynaptic proteins have been directly implicated in neurodegenerative diseases and 4) neuronal dysfunction/synapse loss is known to precede by a substantial period the manifestation of cell death in these diseases. To date, however, there is no established direct evidence of synaptic dysfunction mediating neuronal death during neurodegenerative disease states. The goal of this proposal is to assay synaptic maintenance in two genetic models of neurodegenerative diseases: Drosophila models of Parkinson's Disease (PD), a classic """"""""protein storage"""""""" disease, and Niemann-Pick Type C (NP-C), a classic """"""""lipid storage"""""""" disease. Drosophila was selected for its attractive properties as a new molecular genetic model of neurodegeneration, and its long history as the foremost genetic model for synaptic studies. PD and NP-C were selected as representative of a large number of related neurodegenerative disorders. The Drosophila PD model has been recently established through transgenic over-expression of human alpha-synuclein (a presynaptic protein) and shown to accurately recapitulate the diagnostic features of human PD. A Drosophila model of NP-C is being established through mutation (loss-of-function) of the endogenous NPC I gene, the known cause of human NP-C disease. Specifically, this proposal is to conduct age-progressive studies of synaptic mechanisms in Drosophila PD and NP-C models to correlate synaptic maintenance with the onset, progression and prevalence of neurodegeneration.
The first aim i s to improve Drosophila models by generating fluorescently tagged alpha-synuclein and NPCI proteins whose levels can be reversibly regulated through a temperature-dependent ubiquination strategy. Secondly, to confirm gross features of neurodegeneration in these models with behavioral assays and examination of nervous system/neuronal architecture. Third, and most importantly, to assay synaptic development, function and maintenance in these models. Assays will include electrophysiological measurements of neurotransmission, quantitative fluorescent optical imaging of protein and lipid dynamics in the presynaptic terminal and ultrastructural studies of presynaptic architecture. Together, these studies will allow a conclusive determination of whether synaptic maintenance is compromised in PD and NP-C, and is the causative factor that leads to neuronal cell death and neurodegeneration in these disease states.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
1R01NS041740-01
Application #
6344133
Study Section
Special Emphasis Panel (ZNS1-SRB-K (02))
Program Officer
Murphy, Diane
Project Start
2001-05-01
Project End
2005-04-30
Budget Start
2001-05-01
Budget End
2002-04-30
Support Year
1
Fiscal Year
2001
Total Cost
$374,792
Indirect Cost

  Institution

Name
University of Utah
Department
Biology
Type
Schools of Arts and Sciences
DUNS #
City
Salt Lake City
State
UT
Country
United States
Zip Code
84112

  Publications

Vijayakrishnan, Niranjana; Phillips, Scott E; Broadie, Kendal (2010) Drosophila rolling blackout displays lipase domain-dependent and -independent endocytic functions downstream of dynamin. Traffic 11:1567-78
Kliman, Michal; Vijayakrishnan, Niranjana; Wang, Lily et al. (2010) Structural mass spectrometry analysis of lipid changes in a Drosophila epilepsy model brain. Mol Biosyst 6:958-66
Vijayakrishnan, Niranjana; Woodruff 3rd, Elvin A; Broadie, Kendal (2009) Rolling blackout is required for bulk endocytosis in non-neuronal cells and neuronal synapses. J Cell Sci 122:114-25
Venkatachalam, Kartik; Long, A Ashleigh; Elsaesser, Rebecca et al. (2008) Motor deficit in a Drosophila model of mucolipidosis type IV due to defective clearance of apoptotic cells. Cell 135:838-51
Phillips, Scott E; Woodruff 3rd, E A; Liang, Ping et al. (2008) Neuronal loss of Drosophila NPC1a causes cholesterol aggregation and age-progressive neurodegeneration. J Neurosci 28:6569-82
Haas, Kevin F; Broadie, Kendal (2008) Roles of ubiquitination at the synapse. Biochim Biophys Acta 1779:495-506
Haas, Kevin F; Miller, Stephanie L H; Friedman, David B et al. (2007) The ubiquitin-proteasome system postsynaptically regulates glutamatergic synaptic function. Mol Cell Neurosci 35:64-75
Haas, Kevin F; Woodruff 3rd, Elvin; Broadie, Kendal (2007) Proteasome function is required to maintain muscle cellular architecture. Biol Cell 99:615-26
Trotta, Nick; Orso, Genny; Rossetto, Maria Giovanna et al. (2004) The hereditary spastic paraplegia gene, spastin, regulates microtubule stability to modulate synaptic structure and function. Curr Biol 14:1135-47
Speese, Sean D; Trotta, Nick; Rodesch, Chris K et al. (2003) The ubiquitin proteasome system acutely regulates presynaptic protein turnover and synaptic efficacy. Curr Biol 13:899-910

Showing the most recent 10 out of 11 publications