Recent rodent models for Alzheimer's disease: clinical implications and basic research

Braidy, N; Muñoz P; Palacios, AG; Castellano-Gonzalez, G; Inestrosa, NC; Chung RS; Sachdev P; Guillemin GJ.

Abstract

Alzheimer's disease (AD) is the most common origin of dementia in the elderly. Although the cause of AD remains unknown, several factors have been identified that appear to play a critical role in the development of this debilitating disorder. In particular, amyloid precursor protein (APP), tau hyperphosphorylation, and the secretase enzymes, have become the focal point of recent research. Over the last two decades, several transgenic and non-transgenic animal models have been developed to elucidate the mechanistic aspects of AD and to validate potential therapeutic targets. Transgenic rodent models over-expressing human β-amyloid precursor protein (β-APP) and mutant forms of tau have become precious tools to study and understand the pathogenesis of AD at the molecular, cellular and behavioural levels, and to test new therapeutic agents. Nevertheless, none of the transgenic models of AD recapitulate fully all of the pathological features of the disease. Octodon degu, a South American rodent has been recently found to spontaneously develop neuropathological signs of AD in old age. This review aims to address the limitations and clinical relevance of transgenic rodent models in AD, and to highlight the potential for O. degu as a natural model for the study of AD neuropathology.

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Título según WOS: Recent rodent models for Alzheimer's disease: clinical implications and basic research
Título según SCOPUS: Recent rodent models for Alzheimer's disease: Clinical implications and basic research
Título de la Revista: Journal of Neural Transmission
Volumen: 119
Número: 2
Editorial: Springer-Verlag Wien
Fecha de publicación: 2012
Página de inicio: 173
Página final: 195
Idioma: English
DOI:

10.1007/s00702-011-0731-5

Notas: ISI, SCOPUS - ISI