Abstract

An important questions in research on Alzheimer's Disease (AD) is to define why specific brain regions and neural systems are affected with the progression of the symptoms of dementia and to determine what mechanisms will slow the progression of these processes. This proposal is a continuation of my previous studies aimed at understanding the role of neuro-inflammation in the degeneration of the AD brain. The degeneration or dysfunction of the temporal lobe and forebrain cholinergic neurons are responsible for aspects of the dementia associated with AD and my preliminary studies indicate that temporal lobe and basal forebrain acetylcholine neurons are selectively vulnerable to the neurotoxic effects of chronic neuroinflammation. The current series of studies will examine the effects of chronic neuroinflammation within the brain of four different types of mice: 1) non-transgenic control mice, or transgenic mice that express either, 2) the Swedish mutant amyloid precursor protein, APP (Tg2576; K670N/M671L; Hsiao, et al., 1996), 3) the mutant presenilin type1 (PS1 line 5.1; M146L; Duff, et al, 1996) gene or, 4) both genes simultaneously. The Alzheimer's-like phenotype present in these mice has already been well characterized. The proposed specific aims will test the overall hypothesis that inflammatory proteins influence the pathophysiological processes that underlie the degeneration of neurons in brains of people with AD. I further predict that the extent of pathology induced by the chronic neuroinflammation will be exacerbated in the combined presence of the Beta-amyloid and PS1 mutations. In the present proposal, the biochemical, pathological and behavioral consequences of chronic neuroinflammation produced by the infusion of Iipopolysaccharide (LPS). LPS is a component of the cell wall of gram-negative bacteria and has been used experimentally to stimulate the production of the endogenous cytokines and other inflammatory proteins. Our preliminary studies using LPS infusion into the 4th ventricle, found that the greatest inflammatory response was contained within the basal forebrain, hippocampus, particularly the dentate gyrus, as well as within the entorhinal and piriforin cortexes. The proposed studies will explore the hypothesis that inflammatory processes are involved in the initial stages of cellular and molecular dysfunction that may alter cellular vulnerability and that these changes may in turn lead to cell death and cognitive impairments. In addition, these studies will investigate whether there is an age-associated increase in the vulnerability to these processes. Finally, because the cascade of biochemical processes that leads to neuronal degeneration may involve the production of prostaglandins the proposed studies will also investigate whether it is possible to antagonize these processes and provide neuroprotection. Once accomplished, the research will significantly enhance our understanding of the role of inflammation in neurodegeneration in the AD brain and will greatly improve my ability to reproduce, and then manipulate with potential pharmacotherapies, important steps in the degeneration of neurons in the brain of AD patients.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Project (R01)
Project #
5R01AG010546-10
Application #
6785326
Study Section
Special Emphasis Panel (ZRG1-BDCN-4 (01))
Program Officer
Snyder, Stephen D
Project Start
1994-04-08
Project End
2005-05-31
Budget Start
2004-09-01
Budget End
2005-05-31
Support Year
10
Fiscal Year
2004
Total Cost
$359,813
Indirect Cost

  Institution

Name
University of Arizona
Department
Psychology
Type
Schools of Arts and Sciences
DUNS #
806345617
City
Tucson
State
AZ
Country
United States
Zip Code
85721

  Publications

Rosi, S; Ramirez-Amaya, V; Vazdarjanova, A et al. (2009) Accuracy of hippocampal network activity is disrupted by neuroinflammation: rescue by memantine. Brain 132:2464-77
Marchalant, Yannick; Cerbai, Francesca; Brothers, Holly M et al. (2008) Cannabinoid receptor stimulation is anti-inflammatory and improves memory in old rats. Neurobiol Aging 29:1894-901
Marchalant, Yannick; Brothers, Holly M; Wenk, Gary L (2008) Inflammation and aging: can endocannabinoids help? Biomed Pharmacother 62:212-7
Burke, Sara N; Maurer, Andrew P; Yang, Zhiyong et al. (2008) Glutamate receptor-mediated restoration of experience-dependent place field expansion plasticity in aged rats. Behav Neurosci 122:535-48
Marchalant, Y; Rosi, S; Wenk, G L (2007) Anti-inflammatory property of the cannabinoid agonist WIN-55212-2 in a rodent model of chronic brain inflammation. Neuroscience 144:1516-22
Marriott, L K; McGann-Gramling, K R; Hauss-Wegrzyniak, B et al. (2007) Brain infusion of lipopolysaccharide increases uterine growth as a function of estrogen replacement regimen: suppression of uterine estrogen receptor-alpha by constant, but not pulsed, estrogen replacement. Endocrinology 148:232-40
Rosi, S; Vazdarjanova, A; Ramirez-Amaya, V et al. (2006) Memantine protects against LPS-induced neuroinflammation, restores behaviorally-induced gene expression and spatial learning in the rat. Neuroscience 142:1303-15
Rosi, S; Pert, C B; Ruff, M R et al. (2005) Chemokine receptor 5 antagonist D-Ala-peptide T-amide reduces microglia and astrocyte activation within the hippocampus in a neuroinflammatory rat model of Alzheimer's disease. Neuroscience 134:671-6
Wenk, Gary L; McGann-Gramling, Kristin; Hauss-Wegrzyniak, Beatrice et al. (2004) Attenuation of chronic neuroinflammation by a nitric oxide-releasing derivative of the antioxidant ferulic acid. J Neurochem 89:484-93
Wenk, G L; McGann-Gramling, K; Hauss-Wegrzyniak, B (2004) The presence of the APP(swe) mutation in mice does not increase the vulnerability of cholinergic basal forebrain neurons to neuroinflammation. Neuroscience 125:769-76

Showing the most recent 10 out of 47 publications