Abstract

The identification of the gene (IT-15) causing HD with its expanding CAG triplet repeat clarifies the genetics of HD, but raises many new questions regarding its pathophysiology. The peptide sequence of the putative HD gene protein product has no clear homology to any known protein. Furthermore, the widespread expression of the IT-15 transcript and the lack of notable change in its expression in HD patients raises the issue of how a widely expressed gene can cause selective neuronal vulnerability in restricted portions of the basal ganglia and the cerebral cortex. The studies in this project are designed to elucidate the basic cell biology of the HD protein product (Huntington). Our hypothesis is that the CAG repeats are translated into an expanded polyglutamine tract, causing a gain of function. We have made specific antipeptide affinity purified antibodies to several epitopes within the HD amino acid sequence, for immunochemical and immunohistochemical studies of the protein. We will determine its tissue and regional brain localization. We will study its cellular and subcellular sites of expression using immunohistochemistry and Western blots of subcellular fractions. We will use double label and EM immunohistochemistry in both brain and peripheral tissue. We will express truncated and full length cDNAs with normal and expanded glutamine repeats in expression vectors from which protein can be purified for biochemical studies. In collaborative experiments, we will study the structure of the HD protein. We will elucidate the functional role of the HD protein in stably transfected neuronal cell lines. We will cotransfect the HD protein vector with vectors coding for proteins which associate with it, as identified in the 3rd specific aim. We will use antisense oligonucleotide treated cells and ES cells from gene knockouts to study the function of the normal protein. Finally, we will identify proteins which interact with the HD protein, using coimmunoprecipitation an the yeast two-hybrid system. We will clone full length cDNAs, and study them using techniques described above. These studies taken together will clarity the cellular and tissue sites or expression of the expanding glutamine repeat.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Program Projects (P01)
Project #
2P01NS016375-16A1
Application #
5215124
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
16
Fiscal Year
1996
Total Cost
Indirect Cost

  Publications

Faria, Andreia V; Ratnanather, J Tilak; Tward, Daniel J et al. (2016) Linking white matter and deep gray matter alterations in premanifest Huntington disease. Neuroimage Clin 11:450-460
Krause, Amanda; Mitchell, Claire; Essop, Fahmida et al. (2015) Junctophilin 3 (JPH3) expansion mutations causing Huntington disease like 2 (HDL2) are common in South African patients with African ancestry and a Huntington disease phenotype. Am J Med Genet B Neuropsychiatr Genet 168:573-85
Ross, Christopher A; Pantelyat, Alex; Kogan, Jane et al. (2014) Determinants of functional disability in Huntington's disease: role of cognitive and motor dysfunction. Mov Disord 29:1351-8
Hua, Jun; Unschuld, Paul G; Margolis, Russell L et al. (2014) Elevated arteriolar cerebral blood volume in prodromal Huntington's disease. Mov Disord 29:396-401
Unschuld, Paul G; Liu, Xinyang; Shanahan, Megan et al. (2013) Prefrontal executive function associated coupling relates to Huntington's disease stage. Cortex 49:2661-73
Unschuld, Paul G; Edden, Richard A E; Carass, Aaron et al. (2012) Brain metabolite alterations and cognitive dysfunction in early Huntington's disease. Mov Disord 27:895-902
Guo, Zhihong; Rudow, Gay; Pletnikova, Olga et al. (2012) Striatal neuronal loss correlates with clinical motor impairment in Huntington's disease. Mov Disord 27:1379-86
Fu, Jinrong; Jin, Jing; Cichewicz, Robert H et al. (2012) trans-(-)-?-Viniferin increases mitochondrial sirtuin 3 (SIRT3), activates AMP-activated protein kinase (AMPK), and protects cells in models of Huntington Disease. J Biol Chem 287:24460-72
Rosenblatt, Adam; Kumar, Brahma V; Mo, Alisa et al. (2012) Age, CAG repeat length, and clinical progression in Huntington's disease. Mov Disord 27:272-6
Ratovitski, Tamara; Chighladze, Ekaterine; Arbez, Nicolas et al. (2012) Huntingtin protein interactions altered by polyglutamine expansion as determined by quantitative proteomic analysis. Cell Cycle 11:2006-21

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