Abstract

We propose to form a Drug Discovery Group For the Treatment of Cognitive Impairment Associated with Alzheimer's Disease (DDG-AD). The overall goal is to identify targets that mediate pathogenic molecular events in Alzheimer's Disease (AD), and develop potential drug candidates for AD. The focus of this DDG-AD will be the discovery of distinct neural protease enzymes that mediate abnormal and pathogenic processes in AD, and the development of inhibitors of these proteases as drugs for AD. This DDG-AD will be a highly collaborative effort, integrating many disciplines ranging from chemistry, biochemistry and structural biophysics, to molecular and cellular neurobiology, immunodiagnostics, transgenics and behavioral neuropharmacology. In order to achieve the overall goals of this program, we propose to carry out six scientific projects. In Project 1, probe molecules will be designed to identify target neural proteases, and the three-dimensional structure of these proteases will be solved, enabling rational structure-based drug design. Project 2 will evaluate brain tissue and cerebrospinal fluid to correlate the presence of target neural proteases with the known AD marker, ADAP. Project 2 also will develop diagnostic CSF assays to enable early identification of AD patients. Project 3 will carry out the identification, purification and characterization of unique AD-associated proteases, and establish assay methodology to evaluate target efficacy of designed protease inhibitors. Project 4 will utilize molecular biology-based strategies to establish the molecular basis of abnormal neural protease involvement in AD. Project 4 also will generate DNA constructs for development of transgenic mice that exhibit AD-associated pathology, for use in behavioral studies and drug evaluation. Project 5 will investigate the cellular role of abnormal neural proteases in the processing of amyloid precursor protein, and in other neuronal processes, and will assess the effects of protease inhibitors on these processes. Project 6 will establish the molecular basis for truncation of the nerve growth factor receptor, including the identification of the responsible protease(s), and investigate the role of this process in AD-related neurodegeneration. The six projects will be source tissue for target proteases, and serve as a reference resource for precise clinical identification of disease state (normal, AD, or non-AD dementia). Core C will provide biotechnology support such as protein sequencing, nucleotide sequencing and synthesis, and production of monoclonal antibodies. Core D will support efforts to generate transgenic """"""""Alzheimer's mice"""""""", and evaluate their pathology, in collaboration with Projects 1, 3, 4 and 6. Core F will provide neuropharmacology support to evaluate potential inhibitor candidates, and behavioral evaluation on transgenic mice. The primary research emphasis of this program will be target identification and inhibitor design, however, substantial medicinal chemistry and related activities will be mobilized by Abbott at the appropriate time to expedite development of a clinical drug candidate for AD.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Program Projects (P01)
Project #
5P01AG010481-06
Application #
2051706
Study Section
Neuroscience, Behavior and Sociology of Aging Review Committee (NBSA)
Project Start
1991-09-30
Project End
1996-07-31
Budget Start
1995-08-15
Budget End
1996-07-31
Support Year
6
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
Northwestern University at Chicago
Department
Pharmacology
Type
Schools of Dentistry
DUNS #
005436803
City
Chicago
State
IL
Country
United States
Zip Code
60611

  Publications

Meyer, E M; Tay, E T; Zoltewicz, J A et al. (1998) Neuroprotective and memory-related actions of novel alpha-7 nicotinic agents with different mixed agonist/antagonist properties. J Pharmacol Exp Ther 284:1026-32
Stine Jr, W B; Snyder, S W; Ladror, U S et al. (1996) The nanometer-scale structure of amyloid-beta visualized by atomic force microscopy. J Protein Chem 15:193-203
Bodovitz, S; Klein, W L (1996) Cholesterol modulates alpha-secretase cleavage of amyloid precursor protein. J Biol Chem 271:4436-40
Kohnken, R E; Ladror, U S; Wang, G T et al. (1995) Cathepsin D from Alzheimer's-diseased and normal brains. Exp Neurol 133:105-12
Snyder, S W; Ladror, U S; Wade, W S et al. (1994) Amyloid-beta aggregation: selective inhibition of aggregation in mixtures of amyloid with different chain lengths. Biophys J 67:1216-28
LaDu, M J; Falduto, M T; Manelli, A M et al. (1994) Isoform-specific binding of apolipoprotein E to beta-amyloid. J Biol Chem 269:23403-6
Wang, G T; Ladror, U S; Holzman, T F et al. (1994) Cleavage of fluorogenic substrates for APP-processing proteases by human brain extracts. Ca(2+)-substrate interaction is responsible for Ca2+ stimulation of the neural protease activity. Mol Chem Neuropathol 23:191-9
Ladror, U S; Wang, G T; Klein, W L et al. (1994) Potential beta PP-processing proteinase activities from Alzheimer's and control brain tissues. J Protein Chem 13:357-66
Ladror, U S; Kohnken, R E; Wang, G T et al. (1994) Evidence against a role for the Kunitz domain in amyloidogenic and secretory processing of the amyloid precursor protein. J Neurochem 63:2225-30
Pope, W B; Lambert, M P; Leypold, B et al. (1994) Microtubule-associated protein tau is hyperphosphorylated during mitosis in the human neuroblastoma cell line SH-SY5Y. Exp Neurol 126:185-94

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