Abstract

The clinical project is the translational research arm of the ProgramProject. We have ssembled the largest, fully characterized cohort of families (51) harboring mtDNA mutations. Nearly 90% (44 families)carry a A3243G mutation and the fully symptomatic probands manifest the MELAS phenotype. The family members are assigned to three clinical groups (asymptomatic, oligosymptomatic and fully symptomatic) when first evaluated. Longitudinal and cross- sectional studies of these subjects have provided valuable information regarding natural history. The longitudinal study, now in its 10th year, expands our understanding of the clinical phenotypes and the frequency of medical complications. Key biological variables have been identified that predict increasing morbidity in the asymptomatic/oligosymptomatic group and mortality in the fully symptomatic group. Brain ventricular lactate is the most sensitive biomarker of brain cellular metabolism. Urine sediment DNA is the most reliable measure of mtDNA mutation. Neuropsychological studies show visual memory to be the most vulnerable brain domain. Symptomatic MELAS patients are midway through a three-year, randomized DCA/placebo double-blinded study to determine whether chronic cerebral lactic acidosis contributes to brain injury. We propose three Specific Aims.
Specific Aim #1 continues our natural history study correlating genotype and phenotype.
This aim tests the hypothesis that brain ventricular lactate correlates with clincal phenotype and prognosis.
Specific Aim #2 continues our MELAS/DCA clinical trial.
This aim tests the hypothesis that chronic cerebral lactic acidosis exacerbates the MELAS phenotype.
Specific Aim #3 is a new study assessing early biomarkers of brain dysfunction using PET, fMRI and voxel-based morphometric analysis.
This aim tests the hypothesis that brain ventricular lactate correlates with brain cellular dysfunction. We anticipate that these studies will allow us to determine whether some subjects with the A3243G mutation will remain asymptomatic for the duration of their expected life (low risk group) whereas others who reveal minimal early evidence of structural/functional brain disturbances will become symptomatic and are deserving of early prophylactic treatment (high risk group). The ultimate objective of this clinical project is to find a cure for clinical syndromes associated with mtDNA point mutations.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Program Projects (P01)
Project #
5P01HD032062-12
Application #
7312361
Study Section
Special Emphasis Panel (ZHD1)
Project Start
Project End
Budget Start
2005-12-01
Budget End
2006-11-30
Support Year
12
Fiscal Year
2006
Total Cost
$735,432
Indirect Cost

  Institution

Name
Columbia University (N.Y.)
Department
Type
DUNS #
621889815
City
New York
State
NY
Country
United States
Zip Code
10032

  Publications

Barca, Emanuele; Ganetzky, Rebecca D; Potluri, Prasanth et al. (2018) USMG5 Ashkenazi Jewish founder mutation impairs mitochondrial complex V dimerization and ATP synthesis. Hum Mol Genet 27:3305-3312
Pera, Marta; Larrea, Delfina; Guardia-Laguarta, Cristina et al. (2017) Increased localization of APP-C99 in mitochondria-associated ER membranes causes mitochondrial dysfunction in Alzheimer disease. EMBO J 36:3356-3371
Fryer, Robert H; Bain, Jennifer M; De Vivo, Darryl C (2016) Mitochondrial Encephalomyopathy Lactic Acidosis and Stroke-Like Episodes (MELAS): A Case Report and Critical Reappraisal of Treatment Options. Pediatr Neurol 56:59-61
Varma, Hemant; Faust, Phyllis L; Iglesias, Alejandro D et al. (2016) Whole exome sequencing identifies a homozygous POLG2 missense variant in an infant with fulminant hepatic failure and mitochondrial DNA depletion. Eur J Med Genet 59:540-5
Piekutowska-Abramczuk, Dorota; Kocy?a-Karczmarewicz, Beata; Ma?kowska, Maja et al. (2016) No Evidence for Association of SCO2 Heterozygosity with High-Grade Myopia or Other Diseases with Possible Mitochondrial Dysfunction. JIMD Rep 27:63-8
Cloonan, Suzanne M; Glass, Kimberly; Laucho-Contreras, Maria E et al. (2016) Mitochondrial iron chelation ameliorates cigarette smoke-induced bronchitis and emphysema in mice. Nat Med 22:163-74
Engelstad, Kristin; Sklerov, Miriam; Kriger, Joshua et al. (2016) Attitudes toward prevention of mtDNA-related diseases through oocyte mitochondrial replacement therapy. Hum Reprod 31:1058-65
Ripolone, Michela; Ronchi, Dario; Violano, Raffaella et al. (2015) Impaired Muscle Mitochondrial Biogenesis and Myogenesis in Spinal Muscular Atrophy. JAMA Neurol 72:666-75
Cerutti, Raffaele; Pirinen, Eija; Lamperti, Costanza et al. (2014) NAD(+)-dependent activation of Sirt1 corrects the phenotype in a mouse model of mitochondrial disease. Cell Metab 19:1042-9
Weiduschat, Nora; Kaufmann, Petra; Mao, Xiangling et al. (2014) Cerebral metabolic abnormalities in A3243G mitochondrial DNA mutation carriers. Neurology 82:798-805

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