Abstract

The overall hypothesis addressed by this program is that non-fibrillar aggregated assemblies of amyloid beta (Abeta) which we refer to as Abeta-derived active ligands (ADALs) are active in triggering Alzheimer's disease (AD)-specific cellular responses leading to glial activation, neuronal plasticity malfunction, degeneration and ultimately cell death. We further propose that the generation of these active supramolecular structures of Abeta aggregates can be influenced by the presence of other plaque components, particularly those components derived from glia, and that responses of glial cells contribute to an environment that facilitates and enhances the formationof these bioactive ADALs. Inherent to our hypothesis is that glia are not just appsive bystanders, but are a part of the pathogenesis process. We postulate that Abeta toxicity can be mediated through its effects on glia, that glia-derived proteins can influence the structure of Abeta and its effects on neurons, and that these processes are relevant to the actual neuropathology seen in the AD brain. The questions being addressed in this subproject are: What are the responses of glial cells to ADALs? How do glial proteins affect the formation of ADALs and their bioactivity? Are glia relevant to AD neuropathology? Three aims are proposed to address these questions. 1) The responses of glial cells to ADALs will be evaluated. Specific Abeta aggregates will be prepared and characterized by project 1. We will test the activity of these ADALs on cultures of rat primary astrocytes, by examining the levels and activity of six relevant glial proteins: alpha1-antichymotrypsin (ACT), apolipoprotein E (apoE), apoJ, butyrylcholinesterase (BchE), interleukin-1 (IL-1) and S100beta. 2) The effects of glia on ADAL formation and neurotoxicity will be evaluated. In co-aggregation experiments, we will evaluate the kinetics of aggregate formation and the structure of Abeta aggregates formed in the presence of these six glial proteins willb e correlated with plaque type in AD brain. We willdetermine the regional distribution and immunoreactive density of specific flial proteins in AD and control brain tissue, and establish correlations with the distribution of non-neuritic vs neuritic plaques. This systematic examination should provide insight into how Abeta affects glia, and how glia participate in amyloid plaque progression and development of neurotoxicity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Program Projects (P01)
Project #
5P01AG015501-04
Application #
6340648
Study Section
Project Start
2000-09-01
Project End
2001-08-31
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
4
Fiscal Year
2000
Total Cost
$201,157
Indirect Cost

  Institution

Name
Evanston Hospital
Department
Type
DUNS #
City
Evanston
State
IL
Country
United States
Zip Code
60201

  Publications

Stine Jr, W Blaine; Dahlgren, Karie N; Krafft, Grant A et al. (2003) In vitro characterization of conditions for amyloid-beta peptide oligomerization and fibrillogenesis. J Biol Chem 278:11612-22
Gong, Yuesong; Chang, Lei; Viola, Kirsten L et al. (2003) Alzheimer's disease-affected brain: presence of oligomeric A beta ligands (ADDLs) suggests a molecular basis for reversible memory loss. Proc Natl Acad Sci U S A 100:10417-22
Chromy, Brett A; Nowak, Richard J; Lambert, Mary P et al. (2003) Self-assembly of Abeta(1-42) into globular neurotoxins. Biochemistry 42:12749-60
Wang, Hai-Wei; Pasternak, Joseph F; Kuo, Helen et al. (2002) Soluble oligomers of beta amyloid (1-42) inhibit long-term potentiation but not long-term depression in rat dentate gyrus. Brain Res 924:133-40
Van Eldik, Linda J; Koppal, Tanuja; Watterson, D Martin (2002) Barriers to Alzheimer disease drug discovery and development in academia. Alzheimer Dis Assoc Disord 16 Suppl 1:S18-28
Klein, W L; Krafft, G A; Finch, C E (2001) Targeting small Abeta oligomers: the solution to an Alzheimer's disease conundrum? Trends Neurosci 24:219-24
Guo, L; Sawkar, A; Zasadzki, M et al. (2001) Similar activation of glial cultures from different rat brain regions by neuroinflammatory stimuli and downregulation of the activation by a new class of small molecule ligands. Neurobiol Aging 22:975-81
Koppal, T; Lam, A G; Guo, L et al. (2001) S100B proteins that lack one or both cysteine residues can induce inflammatory responses in astrocytes and microglia. Neurochem Int 39:401-7
Peskind, E R; Griffin, W S; Akama, K T et al. (2001) Cerebrospinal fluid S100B is elevated in the earlier stages of Alzheimer's disease. Neurochem Int 39:409-13
Watterson, D M; Mirzoeva, S; Guo, L et al. (2001) Ligand modulation of glial activation: cell permeable, small molecule inhibitors of serine-threonine protein kinases can block induction of interleukin 1 beta and nitric oxide synthase II. Neurochem Int 39:459-68

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