Abstract

Alzheimer's disease (AD) and Parkinson's Disease (PD) are the most prevalent neurodegenerative diseases (NDD) in America, afflict several million citizens, and represent major sources of disability for the individual and substantial cost to society. The molecular causes of progressive death of cortical and diencephalic neurons in AD and dopamine neurons in PD are not known, nor ar there effective pharmacologic strategies for halting progression of either disease. A recently developed technique (cytoplasmic hybrids= """"""""cybrids"""""""") has allowed genetic transfer of specific mitochondrial electron transport chain (ETC) defects from AD (complex IV) or PD (complex I) platelet mitochondrial DNA into clonal neuronal host cells, showing that the etiology of the ETC defects is in the mitochondrial genome. Cybrid cells provide model systems to explore hypotheses about the causes of cell death resulting from having bioenergetically impaired mitochondria. The experiments in this proposal utilize contemporary microdialysis and molecular techniques to address four Specific Aims that test four hypotheses about the causes of neuronal death in AD and PD.
Aim 1 will characterize the pharmacology of brain hydroxyl free radical (OH*) production following acute, local inhibition of mitochondrial ETC complex I with MPP+ or IV with azide infusion or acute amyloid peptide infusion.
Aim 2 will characterize expression of protective enzyme systems (catalase, glutathione peroxidase, superoxide dismutase) in cybrids derived from AD, PD and control subjects and will determine if exposure of cybrid cells to neurotrophin molecules (NGF, BDNF) alters ROS production and apoptosis following exposure to MPP+ or azide, transcription of genes for protective enzymes, or activities of protective enzymes.
Aim 3 will measure mRNA levels with quantitative RT-PCR and protein levels with Western blotting and/or ELISA for the growth regulatory proteins p53, bcl-2, bcl-xL, and Bax in cybrid cells derived from AD, PD and control subjects during the course of MPP+ azide exposure.
Aim 4 will explore the involvement of bcl- 2, bcl-xL and bax in regulating programmed cell death in cybrid cells derived from AD, PD, or control subjects. Wherever, results in cells will be extended into animals to provide correlation of in vitro with in vivo. The results of experiments in each Specific Aim have potential treatment applications and will provide knowledge applicable to other human neurodegenerative diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Program Projects (P01)
Project #
5P01AG014373-03
Application #
6344593
Study Section
Project Start
2000-09-01
Project End
2002-07-31
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
3
Fiscal Year
2000
Total Cost
$167,919
Indirect Cost

  Institution

Name
University of Virginia
Department
Type
DUNS #
065391526
City
Charlottesville
State
VA
Country
United States
Zip Code
22904

  Publications

Trimmer, Patricia A; Bennett Jr, James P (2009) The cybrid model of sporadic Parkinson's disease. Exp Neurol 218:320-5
Thiffault, Christine; Bennett Jr, James P (2005) Cyclical mitochondrial deltapsiM fluctuations linked to electron transport, F0F1 ATP-synthase and mitochondrial Na+/Ca+2 exchange are reduced in Alzheimer's disease cybrids. Mitochondrion 5:109-19
Onyango, Isaac G; Tuttle, Jeremy B; Bennett Jr, James P (2005) Altered intracellular signaling and reduced viability of Alzheimer's disease neuronal cybrids is reproduced by beta-amyloid peptide acting through receptor for advanced glycation end products (RAGE). Mol Cell Neurosci 29:333-43
Trimmer, Patricia A; Borland, M Kathleen (2005) Differentiated Alzheimer's disease transmitochondrial cybrid cell lines exhibit reduced organelle movement. Antioxid Redox Signal 7:1101-9
Onyango, Isaac G; Tuttle, Jeremy B; Bennett Jr, James P (2005) Brain-derived growth factor and glial cell line-derived growth factor use distinct intracellular signaling pathways to protect PD cybrids from H2O2-induced neuronal death. Neurobiol Dis 20:141-54
Onyango, Isaac G; Bennett Jr, James P; Tuttle, Jeremy B (2005) Endogenous oxidative stress in sporadic Alzheimer's disease neuronal cybrids reduces viability by increasing apoptosis through pro-death signaling pathways and is mimicked by oxidant exposure of control cybrids. Neurobiol Dis 19:312-22
Onyango, Isaac G; Tuttle, Jeremy B; Bennett Jr, James P (2005) Activation of p38 and N-acetylcysteine-sensitive c-Jun NH2-terminal kinase signaling cascades is required for induction of apoptosis in Parkinson's disease cybrids. Mol Cell Neurosci 28:452-61
Trimmer, Patricia A; Keeney, Paula M; Borland, M Kate et al. (2004) Mitochondrial abnormalities in cybrid cell models of sporadic Alzheimer's disease worsen with passage in culture. Neurobiol Dis 15:29-39
Kindler, Dean D; Thiffault, Christine; Solenski, Nina J et al. (2003) Neurotoxic nitric oxide rapidly depolarizes and permeabilizes mitochondria by dynamically opening the mitochondrial transition pore. Mol Cell Neurosci 23:559-73
Dennis, Jameel; Bennett Jr, James P (2003) Interactions among nitric oxide and Bcl-family proteins after MPP+ exposure of SH-SY5Y neural cells II: exogenous NO replicates MPP+ actions. J Neurosci Res 72:89-97

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