Abstract

A deficiency in brain acetylcholine (ACh) function has been implicated in a variety of neurologic and psychiatric disorder. If one were to develop an animal model in which one could simulate the neurochemical conditions which appear to cause these diseases in humans, it would then be feasible to explore mechanisms with which to reverse the situation and to alleviate, and possibly even cure, the specific disease states. This would require the availability of chemical agents which would selectively be taken up in cholinergic nerve terminals, and would subsequently permanently disturb the normal equilibrium of synthetic processes in these nerve terminals. Experiments proposed for the continued support will follow three parallel and integrated lines of research. 1) We will continue to explore the potential of AF64A as an animal model of Alzheimer's disease (AD), and will use it as a probe to attempt to answer mechanistic questions of relevance to cholinergic function in vivo. 2) In addition, a series of new chemical analogs of choline will be synthesized according to specific rationales for their affinity for cholinergic nerve terminals and/or postsynoptic ACh receptors. Following their synthesis the compounds will be screened intensively in mice, rats and cats for their effect on cholinergic systems both in vitro and in vivo. Agents which show promise as potential cholinergic neurotoxins will then be evaluated for specificity toward the cholinergic system, by analyzing the interaction of these promising compounds with the catecholaminergic, serotonergic, and GABA-ergic systems. Histological verification of specific lesions, the effect of these compounds on phospholipid metabolism in brain; and their effects on memory and learning, utilizing sensitive and specific behavioral tests will follow in rats. Tissue cultures obtained from chicks will be utilized for a more extensive evaluation of some of the effects of compound cholinotoxocity, in vitro. 3) Finally, different treatment approaches to reverse AF64A induced cholinergic hypofunction will be tested, utilizing agents such as choline, lecithin, acetylcholinesterase inhibitors; directly acting muscarinic agonists; and combinations of some of these drugs. The outcome of this multiphasic approach will hopefully lead to the development of specific animal models for AD, and to a potential valuable therapy for this disorder.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Research Project (R01)
Project #
5R01MH042572-04
Application #
3381762
Study Section
Neurosciences Research Review Committee (BPN)
Project Start
1986-07-01
Project End
1992-06-30
Budget Start
1989-07-01
Budget End
1992-06-30
Support Year
4
Fiscal Year
1989
Total Cost
Indirect Cost

  Institution

Name
Loyola University Chicago
Department
Type
Schools of Medicine
DUNS #
791277940
City
Maywood
State
IL
Country
United States
Zip Code
60153

  Publications

Santiago, L R; Erickson, L C; Hanin, I (1998) AF64A-induced changes in N-myc expression in the LA-N-2 human neuroblastoma cell line are modulated by choline and hemicholinium-3. Neurochem Res 23:743-50
Santiago, L R; Ivy, M T; Erickson, L C et al. (1995) AF64A-induced cytotoxicity and changes in choline acetyltransferase activity in the LA-N-2 neuroblastoma cell line are modulated by choline and hemicholinium-3. J Neurosci Methods 61:185-90
Dong, X W; Hanin, I; Lorens, S A (1994) AF64A affects septal choline acetyltransferase but not parvalbumin immunoreactive cells. Brain Res Bull 35:217-20
Hortnagl, H; Hansen, L; Kindel, G et al. (1993) Sex differences and estrous cycle-variations in the AF64A-induced cholinergic deficit in the rat hippocampus. Brain Res Bull 31:129-34
Mistry, J S; Abraham, D J; Kozikowski, A P et al. (1991) Neurochemistry of aging. 2. Design, synthesis, and biological evaluation of halomethyl analogues of choline with high affinity choline transport inhibitory activity. J Med Chem 34:2031-6
Chrobak, J J; Napier, T C; Hanin, I et al. (1991) The pharmacology of basal forebrain involvement in cognition. Adv Exp Med Biol 295:383-98
Laganiere, S; Corey, J; Tang, X C et al. (1991) Acute and chronic studies with the anticholinesterase Huperzine A: effect on central nervous system cholinergic parameters. Neuropharmacology 30:763-8
Lorens, S A; Kindel, G; Dong, X W et al. (1991) Septal choline acetyltransferase immunoreactive neurons: dose-dependent effects of AF64A. Brain Res Bull 26:965-71
Hanin, I (1990) AF64A-induced cholinergic hypofunction. Prog Brain Res 84:289-99
Laganiere, S; Marinko, M; Corey, J et al. (1990) Sector-dependent neurotoxicity of ethylcholine aziridinium (AF64A) in the rat hippocampus. Neuropharmacology 29:961-4

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