Abundance of Aß5-x like immunoreactivity in transgenic 5XFAD, APP/PS1KI and 3xTG mice, sporadic and familial Alzheimer's disease.
Mol Neurodegener
; 9: 13, 2014 Apr 02.
Article
em En
| MEDLINE
| ID: mdl-24694184
BACKGROUND: According to the modified amyloid hypothesis the main event in the pathogenesis of Alzheimer's disease (AD) is the deposition of neurotoxic amyloid ß-peptide (Aß) within neurons. Additionally to full-length peptides, a great diversity of N-truncated Aß variants is derived from the larger amyloid precursor protein (APP). Vast evidence suggests that Aßxâ42 isoforms play an important role triggering neurodegeneration due to its high abundance, amyloidogenic propensity and toxicity. Although N-truncated and Aßxâ42 species have been pointed as crucial players in AD etiology, the Aß5-x isoforms have not received much attention. RESULTS: The present study is the first to show immunohistochemical evidence of Aß5-x in familial cases of AD (FAD) and its distribution in APP/PS1KI, 5XFAD and 3xTG transgenic mouse models. In order to probe Aß5-x peptides we generated the AB5-3 antibody. Positive plaques and congophilic amyloid angiopathy (CAA) were observed among all the FAD cases tested carrying either APP or presenilin 1 (PS1) mutations and most of the sporadic cases of AD (SAD). Different patterns of Aß5-x distribution were found in the mouse models carrying different combinations of autosomal mutations in the APP, PS1 and Tau genes. All of them showed extracellular Aß deposits but none CAA. Additionally, they were all affected by a severe amyloid pathology in the hippocampus among other areas. Interestingly, neither 5XFAD nor APP/PS1KI showed any evidence for intraneuronal Aß5-x. CONCLUSIONS: Different degrees of Aß5-x accumulations can be found in the transgenic AD mouse models and human cases expressing the sporadic or the familial form of the disease. Due to the lack of intracellular Aß5-x, these isoforms might not be contributing to early mechanisms in the cascade of events triggering AD pathology. Brain sections obtained from SAD cases showed higher Aß5-x-immunoreactivity in vascular deposits than in extracellular plaques, while both are equally important in the FAD cases. The difference may rely on alternative mechanisms involving Aß5-x peptides and operating in a divergent way in the late and early onset forms of the disease.
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Encéfalo
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Peptídeos beta-Amiloides
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Doença de Alzheimer
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En
Ano de publicação:
2014
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Article