Abstract

Cerebral amyloid angiopathy (CAA) is most commonly associated with vascular deposition of amyloid-beta peptide (Abeta), as well as the presence of advanced glycation endproducts (AGEs), the irreversible products of non-enzymatic glycoxidation. One of the principal means by which Abeta and AGEs impact on vascular function is by interacting with cellular elements, especially endothelial (EC) and smooth muscle (SMC) cells, resulting in changes in cellular properties, and, in certain instances, cell death. Whereas Abeta and AGEs are structurally distinct and derive from different biochemical pathways, they share in common accumulation in CAA and recognition by Receptor for Advanced Glycation Endproducts or RAGE. Engagement of RAGE perturbs cellular functions resulting in sustained oxidant stress, activation of the transport factor NF-kappaB, and, in certain instances, apoptosis. We hypothesize that CAA occurs, in part according to a """"""""two-hit"""""""" model; the first hit is comprised of sustained Abeta/AGE binding to and activation of cellular RAGE; and the second hit includes superimposed environmental challenges such as intermittent ischemia, as in stroke. The focus of Project 3 is to dissect the contribution of RAGE in SMCs to vascular dysfunction in CAA since RAGE is expressed at highest levels in vascular SMC, which is in intimate contact with accumulated Abeta and AGE-modified matrix, and SMCs are known to undergo degeneration in cerebrovascular amyloidosis.
The first aim of Project 3 is to determine if transgenic mice with targeted over expression of wild-type RAGE in SMCs display enhanced vascular perturbation, eventuation in disruption of the vessel wall in Abeta- and/or AGE-rich vascular micro environment.
The second aim i s to determine if transgenic mice with targeted over expression of wild-type RAGE in SMCs display enhanced vascular perturbation, eventuating in disruption of the vessel wall in Abeta-and/or AGE-rich vascular micro environment.
The second aim i s to determine if transgenic mice with targeted over-expression of dominant negative 9DN) RAGE are protected from vascular perturbation by Abeta and AGEs. The long-term goal of Project 3 is to determine the role of RAGE in CAA in order to evaluate whether antagonism of Abeta-AGE interaction with this receptor is a therapeutic target for patients with chronic cerebrovascular dysfunction.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Program Projects (P01)
Project #
5P01AG016223-04
Application #
6588771
Study Section
Project Start
2002-05-01
Project End
2003-04-30
Budget Start
Budget End
Support Year
4
Fiscal Year
2002
Total Cost
Indirect Cost

  Institution

Name
University of Southern California
Department
Type
DUNS #
041544081
City
Los Angeles
State
CA
Country
United States
Zip Code
90033

  Publications

LaRue, Barbra; Hogg, Elizabeth; Sagare, Abhay et al. (2004) Method for measurement of the blood-brain barrier permeability in the perfused mouse brain: application to amyloid-beta peptide in wild type and Alzheimer's Tg2576 mice. J Neurosci Methods 138:233-42
Wu, Ed X; Tang, Haiying; Asai, Tomohiro et al. (2004) Regional cerebral blood volume reduction in transgenic mutant APP (V717F, K670N/M671L) mice. Neurosci Lett 365:223-7
Zlokovic, Berislav V (2004) Clearing amyloid through the blood-brain barrier. J Neurochem 89:807-11
Arancio, Ottavio; Zhang, Hui Ping; Chen, Xi et al. (2004) RAGE potentiates Abeta-induced perturbation of neuronal function in transgenic mice. EMBO J 23:4096-105
Deane, Rashid; Zheng, Wei; Zlokovic, Berislav V (2004) Brain capillary endothelium and choroid plexus epithelium regulate transport of transferrin-bound and free iron into the rat brain. J Neurochem 88:813-20
Deane, Rashid; Wu, Zhenhua; Sagare, Abhay et al. (2004) LRP/amyloid beta-peptide interaction mediates differential brain efflux of Abeta isoforms. Neuron 43:333-44
Deane, Rashid; Wu, Zhenhua; Zlokovic, Berislav V (2004) RAGE (yin) versus LRP (yang) balance regulates alzheimer amyloid beta-peptide clearance through transport across the blood-brain barrier. Stroke 35:2628-31
Tieu, Kim; Perier, Celine; Vila, Miquel et al. (2004) L-3-hydroxyacyl-CoA dehydrogenase II protects in a model of Parkinson's disease. Ann Neurol 56:51-60
Jung, Sonia S; Van Nostrand, William E (2003) Humanin rescues human cerebrovascular smooth muscle cells from Abeta-induced toxicity. J Neurochem 84:266-72
Wu, Zhenhua; Hofman, Florence M; Zlokovic, Berislav V (2003) A simple method for isolation and characterization of mouse brain microvascular endothelial cells. J Neurosci Methods 130:53-63

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