Abstract

application) Alzheimer's disease (AD) is defined by the presence in the brain of a fibrous protein aggregate known as amyloid plaque. Evidence from genetic, pathological, and biochemical studies suggests that amyloid fibril formation may cause neurodegeneration. Inhibition of amyloid formation is therefore a viable strategy for the design of potential AD therapeutic molecules; many industrial programs based on the idea are underway. In order to follow such a strategy, it is necessary to understand the structure of amyloid fibrils and the mechanism by which why form. However, the unusual physical properties of amyloid fibrils preclude their study by widely-applied biophysical methods. This project has as its goal to develop and apply new technology in order to produce a molecular model of AD amyloidogenesis. The model will be used to understand genetic risk factors for AD and to test potential amyloid inhibitors. It is hoped that this model will also allow testable predictions about the AD pathogenic pathway to be made. The group of scientists involved in the program project (the Boston Amyloid group) have a wide variety of backgrounds, ranging from physics to protein chemistry. The investigators, Peter Lansbury, and David Teplow have a history of accomplishment in the protein chemistry of neurodegenerative diseases and are colleagues in the Center for Neurologic Diseases at Bringham and Women's Hospital and Harvard Medical School. Their collaborators include individuals recognized for playing pivotal roles in the development of the three technologies which are the focus of proposal: Robert Griffin (solid state NMR), George Benedek (dynamic light scattering), and Charles Lieher (atomic force microscopy). The collaboration between groups which are focused on the elucidation of a medical problem is required in order to make progress in this difficult area. Another unique and important aspect of this program project is the inclusion of consultants from the pharmaceutical industry who are involved in exploiting amyloid as a therapeutic target. It is hoped that the advisory board will facilitate transfer of new technology to the private sector, where it can be used for the drug discovery process.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Program Projects (P01)
Project #
5P01AG014366-05
Application #
6372100
Study Section
Special Emphasis Panel (ZAG1-BJS-3 (J2))
Program Officer
Snyder, D Stephen
Project Start
1997-06-01
Project End
2003-05-31
Budget Start
2001-07-01
Budget End
2003-05-31
Support Year
5
Fiscal Year
2001
Total Cost
$979,007
Indirect Cost

  Institution

Name
Brigham and Women's Hospital
Department
Type
DUNS #
071723621
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Yong, Winnie; Lomakin, Aleksey; Kirkitadze, Marina D et al. (2002) Structure determination of micelle-like intermediates in amyloid beta -protein fibril assembly by using small angle neutron scattering. Proc Natl Acad Sci U S A 99:150-4
Astrof, Nathan S; Griffin, Robert G (2002) Soft-triple resonance solid-state NMR experiments for assignments of U-13C, 15N labeled peptides and proteins. J Magn Reson 158:157-63
Fezoui, Youcef; Teplow, David B (2002) Kinetic studies of amyloid beta-protein fibril assembly. Differential effects of alpha-helix stabilization. J Biol Chem 277:36948-54
Astrof, N S; Lyon, C E; Griffin, R G (2001) Triple resonance solid state NMR experiments with reduced dimensionality evolution periods. J Magn Reson 152:303-7
Fezoui, Y; Hartley, D M; Harper, J D et al. (2000) An improved method of preparing the amyloid beta-protein for fibrillogenesis and neurotoxicity experiments. Amyloid 7:166-78
Lomakin, A; Benedek, G B; Teplow, D B (1999) Monitoring protein assembly using quasielastic light scattering spectroscopy. Methods Enzymol 309:429-59
Watson, D J; Selkoe, D J; Teplow, D B (1999) Effects of the amyloid precursor protein Glu693-->Gln 'Dutch' mutation on the production and stability of amyloid beta-protein. Biochem J 340 ( Pt 3):703-9
Walsh, D M; Hartley, D M; Kusumoto, Y et al. (1999) Amyloid beta-protein fibrillogenesis. Structure and biological activity of protofibrillar intermediates. J Biol Chem 274:25945-52
Harper, J D; Wong, S S; Lieber, C M et al. (1999) Assembly of A beta amyloid protofibrils: an in vitro model for a possible early event in Alzheimer's disease. Biochemistry 38:8972-80
Teplow, D B (1998) Structural and kinetic features of amyloid beta-protein fibrillogenesis. Amyloid 5:121-42

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