Abstract

The proposed seven year program of research (Leadership and Excellence In Alzheimer's Disease) (LEAD Award) deals entirely with cellular, molecular and genetic aspects of the neurobiology of aging and Alzheimer's disease. The P.I., whose research career has been devoted to genetic approaches to the pathobiology of aging, will focus, in collaboration with two molecular geneticists (K. Fukuchi & S. Deeb), upon a search for genetic loci which can suppress neurotoxicity mediated by the beta amyloid precursor protein. A recently developed embryonal carcinoma cell culture system, in which transfected vectors can be overexpressed in differentiating neural progeny, will be used as a vehicle for the characterization of both known candidate and anonymous cDNA suppressors. Amyloidogenesis and its suppression will also be investigated using a model of inducible overexpression of endogenous wild type or mutant APP. In collaboration with the laboratory of Lee Hartwell, yeast cells will also be employed as vehicles for the detection of cDNA's coding for proteins that interact with specific domains of APP; these too would serve as candidate suppressors of beta amyloidogenesis. Finally, selected suppressors would be biologically assayed in hybrid lines of beta-amyloidogenic transgenic mice (including those developed via the embryonal stem cell route). The discovery of such suppressor loci will have two major applications: 1) as candidate loci for the linkage analysis of various forms of familial AD, the major theme of our ADRC; 2) as a basis for the design of novel preventative and therapeutic agents. The proposal is also designed to nurture the careers of four Assistant Professors. Dr. Margaret Miller (Psychiatry) will be supported for seven years to permit her to extend her investigations of the effects of sex steroid hormones upon the central nervous system of rats, basic research of great potential relevance to patterns of neurobiological aging among millions of American women receiving such exogenous steroids. Pilot studies are proposed by Dr. Glenna Burmer (Pathology) for a method to determine the phase relationships of genetic markers, research that could lead to a major enhancement in the efficiency of linkage analysis in AD and other disorders. Dr. James Thomas (Genetics) will do pilot studies on the genetic control of neuronal stability in the nematode, C. elegans. Dr. Mark Dubach (Psychiatry & Primate Center) will do preliminary tests of the hypothesis that inhibition of lysosomal proteases by leupeptin can lead to beta-amyloidogenesis and other neuropathological stigmata of AD in Macaca fascicularis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Unknown (R35)
Project #
5R35AG010917-04
Application #
2052139
Study Section
Biological and Clinical Aging Review Committee (BCA)
Project Start
1992-09-01
Project End
1999-05-31
Budget Start
1995-06-01
Budget End
1996-05-31
Support Year
4
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
University of Washington
Department
Pathology
Type
Schools of Medicine
DUNS #
135646524
City
Seattle
State
WA
Country
United States
Zip Code
98195

  Publications

Martin, George M (2012) Stochastic modulations of the pace and patterns of ageing: impacts on quasi-stochastic distributions of multiple geriatric pathologies. Mech Ageing Dev 133:107-11
Li, Ge; Cherrier, Monique M; Tsuang, Debby W et al. (2006) Salivary cortisol and memory function in human aging. Neurobiol Aging 27:1705-14
Vidal, J; Verchere, C Bruce; Andrikopoulos, S et al. (2003) The effect of apolipoprotein E deficiency on islet amyloid deposition in human islet amyloid polypeptide transgenic mice. Diabetologia 46:71-9
Hu, Qubai; Cool, Bethany H; Wang, Baiping et al. (2002) A candidate molecular mechanism for the association of an intronic polymorphism of FE65 with resistance to very late onset dementia of the Alzheimer type. Hum Mol Genet 11:465-75
Husseman, J W; Nochlin, D; Vincent, I (2000) Mitotic activation: a convergent mechanism for a cohort of neurodegenerative diseases. Neurobiol Aging 21:815-28
Hu, Q; Jin, L W; Starbuck, M Y et al. (2000) Broadly altered expression of the mRNA isoforms of FE65, a facilitator of beta amyloidogenesis, in Alzheimer cerebellum and other brain regions. J Neurosci Res 60:73-86
Ghatan, S; Larner, S; Kinoshita, Y et al. (2000) p38 MAP kinase mediates bax translocation in nitric oxide-induced apoptosis in neurons. J Cell Biol 150:335-47
Connell-Crowley, L; Le Gall, M; Vo, D J et al. (2000) The cyclin-dependent kinase Cdk5 controls multiple aspects of axon patterning in vivo. Curr Biol 10:599-602
Johnson, M D; Kinoshita, Y; Xiang, H et al. (1999) Contribution of p53-dependent caspase activation to neuronal cell death declines with neuronal maturation. J Neurosci 19:2996-3006
Hu, Q; Hearn, M G; Jin, L W et al. (1999) Alternatively spliced isoforms of FE65 serve as neuron-specific and non-neuronal markers. J Neurosci Res 58:632-40

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