Abstract

Huntington's disease (HD) is a progressive and fatal neurologic disorder caused by an expanded CAG repeat in the gene coding for a protein of unknown function that has been named huntingtin. Recent studies of huntingtin mRNA or protein have given the impression that it is ubiquitously expressed in neurons and so cannot itself explain selective vulnerability. When closely examined, these studies, as well and our preliminary studies, suggest that while most neurons may express huntingtin, there are significant differences in the levels of expression among particular types of neurons and between different intraneuronal compartments. We hypothesize that the neurons most susceptible to neurodegeneration in HD have especially high levels of huntingtin expression. The first goal of this proposal is to characterize the heterogeneity of huntingtin expression in rat brain at the cellular and subcellular level using quantitative immunocytochemical methods. The result will be a detailed picture of its neuronal localization and an understanding of which neuronal processes and organelles are significantly associated with huntingtin. These studies in rat will serve as a basis for our second goal in Aim l which is to characterize the differential localization of huntingtin expression in human brain tissue in distinct neuronal types and to compare controls and HD cases. In particular, we will test our hypothesis that the selectivity of neuronal death in HD can be correlated to differences in huntingtin expression. The exact cause of neuronal death in HD is unknown, however, the leading hypothesis is that of excitotoxicity induced by a defect in energy metabolism that may be caused by oxidative stress.
Our second aim will examine whether cellular markers for oxidative damage (DNA fragmentation, 8-hydroxy deoxyguanosine, malondialdehyde, heme oxygenase, and 3- nitrotyrosine) are increaseD in HD brain; whether they are selectively increased in neurons with the highest levels of huntingtin expression; and whether there is a relationship between the degree of polyglutamine expansion and the degree of oxidative damage. To help determine whether oxidative damage is a primary contributor to neuronal death or a secondary result of neurodegeneration, we will study these same markers in fibroblast cell lines from HD patients and in transfected PC-12 cell lines containing a wide range of CAG repeats. These studies may help establish links between the expression and localization of huntingtin, oxidative stress, and neuronal cell death in HD.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS035255-02
Application #
2669089
Study Section
Special Emphasis Panel (ZRG1-NLS-3 (01))
Program Officer
Oliver, Eugene J
Project Start
1997-03-01
Project End
2000-02-29
Budget Start
1998-03-01
Budget End
1999-02-28
Support Year
2
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Emory University
Department
Neurology
Type
Schools of Medicine
DUNS #
042250712
City
Atlanta
State
GA
Country
United States
Zip Code
30322

  Publications

Fox, Jonathan H; Kama, Jibrin A; Lieberman, Gregory et al. (2007) Mechanisms of copper ion mediated Huntington's disease progression. PLoS One 2:e334
Kazantsev, Aleksey G; Hersch, Steven M (2007) Drug targeting of dysregulated transcription in Huntington's disease. Prog Neurobiol 83:249-59
Hersch, S M; Gevorkian, S; Marder, K et al. (2006) Creatine in Huntington disease is safe, tolerable, bioavailable in brain and reduces serum 8OH2'dG. Neurology 66:250-2
Qiu, Zhihua; Norflus, Fran; Singh, Bhupinder et al. (2006) Sp1 is up-regulated in cellular and transgenic models of Huntington disease, and its reduction is neuroprotective. J Biol Chem 281:16672-80
Gardian, Gabriella; Browne, Susan E; Choi, Dong-Kug et al. (2005) Neuroprotective effects of phenylbutyrate in the N171-82Q transgenic mouse model of Huntington's disease. J Biol Chem 280:556-63
Ferrante, Robert J; Ryu, Hoon; Kubilus, James K et al. (2004) Chemotherapy for the brain: the antitumor antibiotic mithramycin prolongs survival in a mouse model of Huntington's disease. J Neurosci 24:10335-42
Norflus, Fran; Nanje, Agnes; Gutekunst, Claire-Anne et al. (2004) Anti-inflammatory treatment with acetylsalicylate or rofecoxib is not neuroprotective in Huntington's disease transgenic mice. Neurobiol Dis 17:319-25
Christie, Michael A; Hersch, Steven M (2004) Demonstration of nondeclarative sequence learning in mice: development of an animal analog of the human serial reaction time task. Learn Mem 11:720-3
Fox, Jonathan H; Barber, David S; Singh, Bhupinder et al. (2004) Cystamine increases L-cysteine levels in Huntington's disease transgenic mouse brain and in a PC12 model of polyglutamine aggregation. J Neurochem 91:413-22
Hersch, Steven M; Ferrante, Robert J (2004) Translating therapies for Huntington's disease from genetic animal models to clinical trials. NeuroRx 1:298-306

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