Abstract

The present proposal will investigate the role of mitochondrial dysfunction and oxidative damage in several transgenic mouse models of neurodegenerative diseases. In particular we will investigate whether mice with a deficiency in dihydrolipoamide dehydrogenase will show increased oxidative damage, increased vulnerability to mitochondrial toxins and when crossed to transgenic mouse models of Alzheimer's disease (AD), Huntington's disease (HD), spinocerebellar ataxia1 (sca1) and dentatorubropallidoluysian atrophy (DRPLA) whether this will accelerate the phenotype. The mice with a deficiency of murine dihydrolipoamide dehydrogenase show deficiencies in several mitochondrial enzymes including a 50% deficiency in both pyruvate dehydrogenase and alpha-ketoglutarate dehydrogenase. They will therefore help to test the potential role of reduced levels of these enzymes in neurodegenerative diseases. We will also carry out studies of mitochondrial oxygen utilization, oxidative damage and of the mitochondrial permeability transition in transgenic mouse models of HD, SCA1 and DRPLA. Another theme of the present program project grant is that increased transglutaminase activity may contribute to neuronal dysfunction and the development of cytoplasmic and nuclear inclusions in transgenic mouse models of HD, SCA1 and DRPLA. We will therefore measure brain transglutaminase activity as well as epsilon(4-glutamyl) lysine in brains of transgenic mouse models of these illnesses in collaboration with project 4. We will also test whether tissue transglutaminase inhibitors can extend survival and block the development of the intranuclear inclusions. We will also investigate whether transgenic mice with mutations in the amyloid precursor protein exhibit metabolic abnormalities in oxidative damage. Lastly if oxidative damage plays a role in the pathogenesis of neurodegenerative diseases then crossing transgenic ADP, HD, SCA1 or DRPLA mice with transgenic mice deficient in manganese SOD or glutathione peroxidase should accelerate the phenotype. We will therefore look at defects on survival as well as on markers of oxidative damage in mice following these crosses. The proposed studies will help to elucidate the role of mitochondrial dysfunction in transgenic mouse models of both AD as well as HD, SCA1 and DRPLA. They may also lead to novel and useful treatment strategies for these disorders.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Program Projects (P01)
Project #
5P01AG014930-02
Application #
6336231
Study Section
National Institute on Aging Initial Review Group (NIA)
Project Start
2000-08-01
Project End
2001-05-31
Budget Start
Budget End
Support Year
2
Fiscal Year
2000
Total Cost
$181,206
Indirect Cost

  Institution

Name
Winifred Masterson Burke Med Research Institute
Department
Type
DUNS #
780676131
City
White Plains
State
NY
Country
United States
Zip Code
10605

  Publications

Tapias, Victor; Jainuddin, Shari; Ahuja, Manuj et al. (2018) Benfotiamine treatment activates the Nrf2/ARE pathway and is neuroprotective in a transgenic mouse model of tauopathy. Hum Mol Genet 27:2874-2892
Garg, Ankur; Hannan, Abdul; Wang, Qian et al. (2018) FGF-induced Pea3 transcription factors program the genetic landscape for cell fate determination. PLoS Genet 14:e1007660
Franich, Nicholas R; Basso, Manuela; André, Emily A et al. (2018) Striatal Mutant Huntingtin Protein Levels Decline with Age in Homozygous Huntington's Disease Knock-In Mouse Models. J Huntingtons Dis 7:137-150
Karuppagounder, Saravanan S; Zhai, Yujia; Chen, Yingxin et al. (2018) The interferon response as a common final pathway for many preconditioning stimuli: unexpected crosstalk between hypoxic adaptation and antiviral defense. Cond Med 1:143-150
Gibson, Gary E; Thakkar, Ankita (2017) Interactions of Mitochondria/Metabolism and Calcium Regulation in Alzheimer's Disease: A Calcinist Point of View. Neurochem Res 42:1636-1648
Gureev, Artem P; Shaforostova, Ekaterina A; Starkov, Anatoly A et al. (2017) Simplified qPCR method for detecting excessive mtDNA damage induced by exogenous factors. Toxicology 382:67-74
Ratan, Rajiv R (2017) Building on NeuroNEXT: Next generation clinics to cure chronic neurological disability. Ann Neurol 82:859-862
Starkov, Anatoly A; Chinopoulos, Christos; Starkova, Natalia N et al. (2017) Divalent cation chelators citrate and EDTA unmask an intrinsic uncoupling pathway in isolated mitochondria. J Bioenerg Biomembr 49:3-11
Chen, Huanlian; Xu, Hui; Potash, Samuel et al. (2017) Mild metabolic perturbations alter succinylation of mitochondrial proteins. J Neurosci Res 95:2244-2252
Shurubor, Yevgeniya I; D'Aurelio, Marilena; Clark-Matott, Joanne et al. (2017) Determination of Coenzyme A and Acetyl-Coenzyme A in Biological Samples Using HPLC with UV Detection. Molecules 22:

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