Aging, microglia and cytoskeletal regulation are key factors in the pathological evolution of the APP23 mouse model for Alzheimer's disease

Leen Janssen, Marissa L. Dubbelaar, Inge R. Holtman, Jelkje de Boer-Bergsma, Bart J. L. Eggen, Hendrikus W. G. M. Boddeke, Peter P. De Deyn, Debby Dam, van

OnderzoeksoutputAcademicpeer review

10 Citaten (Scopus)
319 Downloads (Pure)

Samenvatting

Aging is the key risk factor for Alzheimer's disease (AD). In addition, the amyloid-beta (A beta) peptide is considered a critical neurotoxic agent in AD pathology. However, the connection between these factors is unclear. We aimed to provide an extensive characterization of the gene expression profiles of the amyloidosis APP23 model for AD and control mice and to evaluate the effect of aging on these profiles. We also correlated our findings to changes in soluble A beta-levels and other pathological and symptomatic features of the model. We observed a clear biphasic expression profile. The first phase displayed a maturation profile, which resembled features found in young carriers of familial AD mutations. The second phase reflected aging processes and showed similarities to the progression of human AD pathology. During this phase, the model displayed a clear upregulation of microglial activation and lysosomal pathways and downregulation of neuron differentiation and axon guidance pathways. Interestingly, the changes in expression were all correlated to aging in general, but appeared more extensive/accelerated in APP23 mice. (C) 2016 Elsevier B.V. All rights reserved.

Originele taal-2English
Pagina's (van-tot)395-405
Aantal pagina's11
TijdschriftBiochimica et biophysica acta-Molecular basis of disease
Volume1863
Nummer van het tijdschrift2
DOI's
StatusPublished - feb.-2017

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