Abstract

This application is designed to address the hypothesis that elevations in the lesion equilibrium in mitochondrial DNA (mtDNA) following oxidative damage is an early key factor that sets in motion the cascade of events that ultimately leads to the phenotypes associated with aging and certain neurodegenerative diseases. Specifically, we will focus on factors that are involved in disruption of the normal lesion equilibrium in mtDNA which exists between the formation of oxidative damage and its subsequent removal by repair processes. Additionally, we will explore some of the consequences resulting from changes in the lesion equilibrium. This will be accomplished through the pursuit of four specific aims. The first and second aims are designed to determine how repair mechanisms in neurons affect the re-establishment of the normal lesion equilibrium in mtDNA. These studies will employ cultures of different types of neurons to answer questions relating to the hypothesis that the ability of neurons to repair lesions in their mtDNA is a key component in the maintenance of a normal lesion equilibrium. Defects in this repair allow the lesion equilibrium to rise out of control and initiate some of the phenotypes associated with aging and neurodegenerative diseases.
The third aim will evaluate the effects of recombinant DNA repair proteins targeted to the mitochondria. These studies will use primary cultures of neurons that are transfected with genes that encode mtDNA repair enzymes. These proteins will modulate mtDNA repair capacity and directly alter the lesion equilibrium in mtDNA act as an early key factor that ultimately leads to cellular dysfunction and death.
The final aim i s structured to determine regional differences in levels of oxidative damage in mtDNA in transgenic animal model of chronic oxidative stress. These studies will use these mice to explore the hypothesis that specific aims in the brain are more vulnerable to oxidative damage in mtDNA. This increased damage is predominantly in certain nucleotide """"""""hot spots"""""""" which ultimately become mutated and contribute to phenotypes associated with aging and the pathogenesis of neurodegenerative disorders. When successfully completed, these studies will provide a more thorough understanding of the role that mtDNA damage and its subsequent repair can play in aging and the pathogenesis of some neurodegenerative diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Project (R01)
Project #
1R01AG019602-01
Application #
6352361
Study Section
Special Emphasis Panel (ZAG1-BJB-8 (M2))
Program Officer
Wise, Bradley C
Project Start
2000-09-30
Project End
2005-08-31
Budget Start
2000-09-30
Budget End
2001-08-31
Support Year
1
Fiscal Year
2000
Total Cost
$240,331
Indirect Cost

  Institution

Name
University of South Alabama
Department
Biology
Type
Schools of Medicine
DUNS #
City
Mobile
State
AL
Country
United States
Zip Code
36688

  Publications

Druzhyna, Nadiya M; Wilson, Glenn L; LeDoux, Susan P (2008) Mitochondrial DNA repair in aging and disease. Mech Ageing Dev 129:383-90
Pastukh, Viktoriya; Shokolenko, Inna N; Wilson, Glenn L et al. (2008) Mutations in the passenger polypeptide can affect its partitioning between mitochondria and cytoplasm: mutations can impair the mitochondrial import of DsRed. Mol Biol Rep 35:215-23
Alexeyev, M F; Venediktova, N; Pastukh, V et al. (2008) Selective elimination of mutant mitochondrial genomes as therapeutic strategy for the treatment of NARP and MILS syndromes. Gene Ther 15:516-23
Ho, Renee; Rachek, Lyudmila I; Xu, Yi et al. (2007) Yeast apurinic/apyrimidinic endonuclease Apn1 protects mammalian neuronal cell line from oxidative stress. J Neurochem 102:13-24
Harrison, Jason F; Rinne, Mikael L; Kelley, Mark R et al. (2007) Altering DNA base excision repair: use of nuclear and mitochondrial-targeted N-methylpurine DNA glycosylase to sensitize astroglia to chemotherapeutic agents. Glia 55:1416-25
LeDoux, S P; Druzhyna, N M; Hollensworth, S B et al. (2007) Mitochondrial DNA repair: a critical player in the response of cells of the CNS to genotoxic insults. Neuroscience 145:1249-59
Pastukh, Viktoriya; Shokolenko, Inna; Wang, Bin et al. (2007) Human mitochondrial transcription factor A possesses multiple subcellular targeting signals. FEBS J 274:6488-99
Rachek, L I; Musiyenko, S I; LeDoux, S P et al. (2007) Palmitate induced mitochondrial deoxyribonucleic acid damage and apoptosis in l6 rat skeletal muscle cells. Endocrinology 148:293-9
Rachek, Lyudmila I; Thornley, Nancy P; Grishko, Valentina I et al. (2006) Protection of INS-1 cells from free fatty acid-induced apoptosis by targeting hOGG1 to mitochondria. Diabetes 55:1022-8
Rachek, Lyudmila I; Grishko, Valentina I; Ledoux, Susan P et al. (2006) Role of nitric oxide-induced mtDNA damage in mitochondrial dysfunction and apoptosis. Free Radic Biol Med 40:754-62

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