Abstract

Available evidence implicates genetics as a major risk factor in Alzheimer disease. Multiple reports of molecular and cellular abnormalities in non-neural tissues including cultured cells suggest that the expression of the predisposing gene(s) is not restricted to the nervous system. Previous studies have indicated changes in glucose and energy metabolism in both brain and cultured skin fibroblasts in Alzheimer disease. This project will elucidate the bases of these changes in cultured cells. Initial studies will test whether alterations of glucose metabolism, similar to those already identified in preliminary studies, distinguish between fibroblasts from groups of affected individuals and unaffected older members of the large Alzheimer kindreds available to us. Those aspects of the complex metabolic pathways of glucose and glutamine primarily contributing to the observed alterations will be determined from the relative incorporation of radiolabelled substrates into C02 and lactate and from direct measures of mitochondrial changes using oxygen uptake. Based on the results of these studies, specific metabolites and enzymes will be assayed to test whether changes are attributable to identifiable defects of individual components within the affected pathways. The effect of the metabolic changes on cellular function (which could ultimately compromise cell survival) will be determined from the content of energy- related metabolites (adenine nucleotides and phosphocreatine) and critical metabolic parameters (from the above studies) under normal conditions and during metabolic """"""""stress"""""""" (in the presence of uncoupling agent or altered substrate availability). 2- Deoxyglucose uptake (as a convenient marker of glucose metabolism) or other more sensitive parameters identified in the above studies will be used to determine whether metabolic defects in the Alzheimer fibroblasts are an exacerbation of normal age-related changes, and whether similar changes are seen in other neurological diseases. The identification of diagnostic markers in Alzheimer cells and/or the identification of specific metabolic abnormalities would be a major advance in understanding the pathogenesis of this disease and may be an important step in the development of specific treatments.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Program Projects (P01)
Project #
5P01AG003853-07
Application #
3813780
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
7
Fiscal Year
1989
Total Cost
Indirect Cost

  Institution

Name
Burke Rehabilitation Center (White Plns,NY)
Department
Type
DUNS #
City
White Plains
State
NY
Country
United States
Zip Code
10605

  Publications

Ko, L W; Sheu, K F; Thaler, H T et al. (2001) Selective loss of KGDHC-enriched neurons in Alzheimer temporal cortex: does mitochondrial variation contribute to selective vulnerability? J Mol Neurosci 17:361-9
Nolan, K A; Lino, M M; Seligmann, A W et al. (1998) Absence of vascular dementia in an autopsy series from a dementia clinic. J Am Geriatr Soc 46:597-604
Bernstein, J J; Karp, S M; Goldberg, W J et al. (1996) Human leptomeningeal-derived cells express GFAP and HLADR when grafted into rat spinal cord. Int J Dev Neurosci 14:681-7
Calingasan, N Y; Bernstein, J J; Blass, J P (1996) Absence of neuronal and glial proteins in human and rat leptomeninges in situ. J Neurol Sci 144:21-3
Makar, T K; Cooper, A J; Tofel-Grehl, B et al. (1995) Carnitine, carnitine acetyltransferase, and glutathione in Alzheimer brain. Neurochem Res 20:705-11
Black, R S; DeGiorgio, L A; Sheu, K F et al. (1994) Expression of neuronal proteins in cells from normal adult rat brain propagated in serial culture. J Neurochem 62:2132-40
DeGiorgio, L A; Sheu, K F; Blass, J P (1994) Culture from human leptomeninges of cells containing neurofilament protein and neuron-specific enolase. J Neurol Sci 124:141-8
Blass, J P; Markesbery, W R; Ko, L W et al. (1994) Presence of neuronal proteins in serially cultured cells from autopsy human brain. J Neurol Sci 121:132-8
Huang, H M; Martins, R; Gandy, S et al. (1994) Use of cultured fibroblasts in elucidating the pathophysiology and diagnosis of Alzheimer's disease. Ann N Y Acad Sci 747:225-44
Sheu, K F; Cooper, A J; Koike, K et al. (1994) Abnormality of the alpha-ketoglutarate dehydrogenase complex in fibroblasts from familial Alzheimer's disease. Ann Neurol 35:312-8

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