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Publication : Synergistic Effect on Neurodegeneration by N-Truncated Aβ<sub>4-42</sub> and Pyroglutamate Aβ<sub>3-42</sub> in a Mouse Model of Alzheimer's Disease.

First Author  Lopez-Noguerola JS Year  2018
Journal  Front Aging Neurosci Volume  10
Pages  64 PubMed ID  29568268
Mgi Jnum  J:274992 Mgi Id  MGI:6306012
Doi  10.3389/fnagi.2018.00064 Citation  Lopez-Noguerola JS, et al. (2018) Synergistic Effect on Neurodegeneration by N-Truncated Abeta4-42 and Pyroglutamate Abeta3-42 in a Mouse Model of Alzheimer's Disease. Front Aging Neurosci 10:64
abstractText  The N-terminally truncated pyroglutamate Abeta3-42 (AbetapE3-42) and Abeta4-42 peptides are known to be highly abundant in the brain of Alzheimer's disease (AD) patients. Both peptides show enhanced aggregation and neurotoxicity in comparison to full-length Abeta, suggesting that these amyloid peptides may play an important role in the pathogenesis of AD. The aim of the present work was to study the direct effect of the combination of AbetapE3-42 and Abeta4-42 on ongoing AD-related neuron loss, pathology, and neurological deficits in transgenic mice. Bigenic mice were generated by crossing the established TBA42 and Tg4-42 mouse models expressing the N-truncated Abeta peptides AbetapE3-42 and Abeta4-42, respectively. After generation of the bigenic mice, detailed phenotypical characterization was performed using either immunostainings to evaluate amyloid pathology or quantification of neuron numbers using design-based stereology. The elevated plus maze was used to study anxiety levels. In order to evaluate sensori-motor deficits, the inverted grid, the balance beam and the string suspension tasks were applied. We could demonstrate that co-expression of AbetapE3-42 and Abeta4-42 accelerates neuron loss in the CA1 pyramidal layer of young bigenic mice as seen by reduced neuron numbers in comparison to single transgenic homozygous mice expressing either AbetapE3-42 or Abeta4-42. This observation coincides with the robust intraneuronal Abeta accumulation observed in the bigenic mice. In addition, loss of anxiety and motor deficits were enhanced in an age-dependent manner. The sensori-motor deficits correlate with the abundant spinal cord pathology, as demonstrated by robust intracellular Abeta accumulation within motor neurons and extracellular Abeta deposition. Our observations demonstrate that a combination of AbetapE3-42 and Abeta4-42 has a stronger effect on ongoing AD pathology than the peptides alone. Therefore, AbetapE3-42 and Abeta4-42 might represent excellent potential therapeutic targets and diagnostic markers for AD.
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