Abstract

As a researcher trained in clinical neurology and basic science with a primary interests in the field of mitochondrial disorders, my principal scientific goal is to better understand the pathogenic mechanisms of this group of diseases and to identify strategies to treat them. My main scientific career goals are to make novel and important contributions to the field of mitochondrial disorders and to satisfy the requirements to become a tenured faculty member in a prestigious academic institution. I believe that the Department of Neurology and Neuroscience at the Weill medical College is an ideal environment to conduct my work and to fulfill my career goals because it provides a fertile ground for scientific growth by allowing interactions with topnotch scientists within the tri-institutional organization that includes Cornell University, Memorial Sloan Kettering, and Rockefeller University. The scope of this proposal is twofold. First, to modulate mitochondrial ATP synthesis in the syndrome NARP (neuropathy ataxia and retinitis pigmentosa) caused by mutations in the mtDNA encoded ATPase 6 (A6). Second, to develop cellular and animal models recapitulating the features of NARP. Such models will serve to investigate in vivo the pathogenic mechanisms underlying mitochondrial disorders and to test therapeutic approaches.
Aim 1 : NARP cells generate increased free radicals. The mitochondrial respiratory chain is defective presumably due to damage or inhibition and ATP synthesis in NARP cybrid cells can be improved by antioxidants. We will define the mechanisms underlying the respiratory chain dysfunction and test the effects of antioxidants in cells directly derived from NARP patients.
Aim 2 : We showed that the expression of a wild type A6 protein allotopically from the nucleus improved mitochondrial ATP synthesis in a cybrid model of NARP. The goal is to assess whether allotopic expression of A6 will improve ATP synthesis in patient-derived cells and whether this approach can have a therapeutic use.
Aim 3 : There are no animal models of NARP. Exogenous mtDNA cannot be transferred into mitochondria to generate transgenic models of NARP. We will test two alternative strategies to generate mutants that recapitulate the biochemical and clinical defects of NARP: a) By allotopic expression from the nucleus of a mutant A6 targeted to normal mitochondria; b) By introducing mutations in a nuclear-encoded mitochondrial protein, ATPase subunit C, at crucial sites of interaction with A6.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Scientist Development Award - Research (K02)
Project #
5K02NS047306-03
Application #
7113662
Study Section
Special Emphasis Panel (ZNS1-SRB-M (07))
Program Officer
Golanov, Eugene V
Project Start
2004-09-15
Project End
2009-08-31
Budget Start
2006-09-01
Budget End
2007-08-31
Support Year
3
Fiscal Year
2006
Total Cost
$171,504
Indirect Cost

  Institution

Name
Weill Medical College of Cornell University
Department
Neurology
Type
Schools of Medicine
DUNS #
060217502
City
New York
State
NY
Country
United States
Zip Code
10065

  Publications

Yang, Hua; Brosel, Sonja; Acin-Perez, Rebeca et al. (2010) Analysis of mouse models of cytochrome c oxidase deficiency owing to mutations in Sco2. Hum Mol Genet 19:170-80
D'Aurelio, M; Vives-Bauza, C; Davidson, M M et al. (2010) Mitochondrial DNA background modifies the bioenergetics of NARP/MILS ATP6 mutant cells. Hum Mol Genet 19:374-86
Acin-Perez, Rebeca; Hoyos, Beatrice; Zhao, Feng et al. (2010) Control of oxidative phosphorylation by vitamin A illuminates a fundamental role in mitochondrial energy homoeostasis. FASEB J 24:627-36
Acin-Perez, Rebeca; Salazar, Eric; Brosel, Sonja et al. (2009) Modulation of mitochondrial protein phosphorylation by soluble adenylyl cyclase ameliorates cytochrome oxidase defects. EMBO Mol Med 1:392-406
Acin-Perez, Rebeca; Salazar, Eric; Kamenetsky, Margarita et al. (2009) Cyclic AMP produced inside mitochondria regulates oxidative phosphorylation. Cell Metab 9:265-76
Vives-Bauza, Cristofol; Anand, Monika; Shirazi, Arash K et al. (2008) The age lipid A2E and mitochondrial dysfunction synergistically impair phagocytosis by retinal pigment epithelial cells. J Biol Chem 283:24770-80
Kwong, Jennifer Q; Henning, Matthew S; Starkov, Anatoly A et al. (2007) The mitochondrial respiratory chain is a modulator of apoptosis. J Cell Biol 179:1163-77
Vives-Bauza, Cristofol; Yang, Lichuan; Manfredi, Giovanni (2007) Assay of mitochondrial ATP synthesis in animal cells and tissues. Methods Cell Biol 80:155-71
D'Aurelio, Marilena; Gajewski, Carl D; Lenaz, Giorgio et al. (2006) Respiratory chain supercomplexes set the threshold for respiration defects in human mtDNA mutant cybrids. Hum Mol Genet 15:2157-69