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Journal of Experimental Neurology

ISSN: 2692-2819

Review Article Open Access
Volume 5 | Issue 2 | DOI: https://doi.org/10.33696/Neurol.5.087

Cerebrovascular Dysfunction in Alzheimer’s Disease and Transgenic Rodent Models

Xing Fang1, Fan Fan2, Jane J Border1, Richard J. Roman1,*
  • 1Department of Pharmacology and Toxicology, University of Mississippi Medical Center, Jackson, MS 39216, USA
  • 2Department of Physiology, Augusta University, Augusta, GA 30912, USA
+ Affiliations - Affiliations

Corresponding Author

Richard J. Roman, rroman@umc.edu

Received Date: December 14, 2023

Accepted Date: January 24, 2024

Citation:

Fang X, Fan F, Border JJ, Roman RJ. Cerebrovascular Dysfunction in Alzheimer’s Disease and Transgenic Rodent Models. J Exp Neurol. 2024;5(2):42-64.


Copyright: © 2024 Fang X, et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

Abstract

Alzheimer’s Disease (AD) and Alzheimer’s Disease-Related Dementia (ADRD) are the primary causes of dementia that has a devastating effect on the quality of life and is a tremendous economic burden on the healthcare system. The accumulation of extracellular beta-amyloid (Aβ) plaques and intracellular hyperphosphorylated tau-containing neurofibrillary tangles (NFTs) in the brain are the hallmarks of AD. They are also thought to be the underlying cause of inflammation, neurodegeneration, brain atrophy, and cognitive impairments that accompany AD. The discovery of APP, PS1, and PS2 mutations that increase Aβ production in families with early onset familial AD led to the development of numerous transgenic rodent models of AD. These models have provided new insight into the role of Aβ in AD; however, they do not fully replicate AD pathology in patients. Familial AD patients with mutations that elevate the production of Aβ represent only a small fraction of dementia patients. In contrast, those with late-onset sporadic AD constitute the majority of cases. This observation, along with the failure of previous clinical trials targeting Aβ or Tau and the modest success of recent trials using Aβ monoclonal antibodies, has led to a reappraisal of the view that Aβ accumulation is the sole factor in the pathogenesis of AD. More recent studies have established that cerebral vascular dysfunction is one of the earliest changes seen in AD, and 67% of the candidate genes linked to AD are expressed in the cerebral vasculature. Thus, there is an increasing appreciation of the vascular contribution to AD, and the National Institute on Aging (NIA) and the Alzheimer’s Disease Foundation recently prioritized it as a focused research area. This review summarizes the strengths and limitations of the most commonly used transgenic AD animal models and current views about the contribution of Aβ accumulation versus cerebrovascular dysfunction in the pathogenesis of AD. 

Keywords

Alzheimer’s disease, Brain hypoperfusion, Beta-amyloid, Tau, Cerebrovascular dysfunction, Neurovascular coupling, AD animal models

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