Abstract

The central hypothesis to be tested in the proposed studies is that key cellular abnormalities in Alzheimer's disease are expressed in and can usefully be studied at the cellular level in non-neural tissues as well as the brain. The studies focus on tissue culture models and specifically cultured skin fibroblasts. Project 1 will test the validity and utility of a culture system in which fibroblasts appear to express antigens normally associated with neurons in culture or in vivo (neuron-specific enolase [NSE] and neurofilaments [NF]), and in which a significantly higher proportion of fibroblasts from Alzheimer patients react with antibodies to paired helical filaments than do cells from controls. The molecules responsible for these reactions will be characterized. The relation of the accumulation of those molecules to biological age in culture and to mitochondrial and other metabolic abnormalities described in Alzheimer cells will be determined, and the clinical specificity and diagnostic utility of this observation tested. Project 2 will examine signal transduction mechanisms in homeostasis, the inositol phosphate cascade, and cyclic AMP). The emphasis will be on elucidating basic mechanisms including relationships to biological age and to mechanisms studied in Project 1. Project 5 will compare mitochondrial metabolism in Alzheimer and control cells, determining the mechanisms underlying the reported mitochondrial abnormalities and particularly the fragility in Alzheimer and control cells, following up on reports of abnormal DNA repair. Project 7 will define the mechanisms underlying the loss of neuropeptide plasticity in aging superior cervical neurons in culture; it relates to the other studies, since age-is a major risk factor Alzheimer's disease. A clinical Pilot Project will examine writing abnormalities in Alzheimer patients. The cores will provide support activities, including the provision for all studies of fibroblasts of cells grown under meticulously controlled conditions, with Alzheimer and control cells matched for biological age in culture as well as chronological age and gender of donor.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Program Projects (P01)
Project #
7P01AG003853-09
Application #
3090718
Study Section
Aging Review Committee (AGE)
Project Start
1983-06-01
Project End
1993-05-31
Budget Start
1991-06-01
Budget End
1992-05-31
Support Year
9
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
Winifred Masterson Burke Med Research Institute
Department
Type
DUNS #
780676131
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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