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Prinzen, C.* ; Trümbach, D. ; Wurst, W. ; Endres, K.* ; Postina, R.* ; Fahrenholz, F.*

Differential gene expression in ADAM10 and mutant ADAM10 transgenic mice.

BMC Genomics 10:66 (2008)
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Open Access Gold
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Background: In a transgenic mouse model of Alzheimer disease (AD), cleavage of the amyloid precursor protein (APP) by the alpha-secretase ADAM10 prevented amyloid plaque formation, and alleviated cognitive deficits. Furthermore, ADAM10 overexpression increased the cortical synaptogenesis. These results suggest that upregulation of ADAM10 in the brain has beneficial effects on AD pathology. Results: To assess the influence of ADAM10 on the gene expression profile in the brain, we performed a microarray analysis using RNA isolated from brains of five months old mice overexpressing either the alpha-secretase ADAM10, or a dominant-negative mutant (dn) of this enzyme. As compared to non-transgenic wild-type mice, in ADAM10 transgenic mice 355 genes, and in dnADAM10 mice 143 genes were found to be differentially expressed. A higher number of genes was differentially regulated in double-transgenic mouse strains additionally expressing the human APP([V717I]) mutant. Overexpression of proteolytically active ADAM10 affected several physiological pathways, such as cell communication, nervous system development, neuron projection as well as synaptic transmission. Although ADAM10 has been implicated in Notch and beta-catenin signaling, no significant changes in the respective target genes were observed in adult ADAM10 transgenic mice. Real-time RT-PCR confirmed a downregulation of genes coding for the inflammation-associated proteins S100a8 and S100a9 induced by moderate ADAM10 overexpression. Overexpression of the dominant-negative form dnADAM10 led to a significant increase in the expression of the fatty acid-binding protein Fabp7, which also has been found in higher amounts in brains of Down syndrome patients. Conclusion: In general, there was only a moderate alteration of gene expression in ADAM10 overexpressing mice. Genes coding for pro-inflammatory or pro-apoptotic proteins were not over-represented among differentially regulated genes. Even a decrease of inflammation markers was observed. These results are further supportive for the strategy to treat AD by increasing the alpha-secretase activity.
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Publikationstyp Artikel: Journalartikel
Dokumenttyp Wissenschaftlicher Artikel
Schlagwörter amyloid precursor protein; heparin-binding domain; growth-factor-i; alzheimers-disease; over-expression; cell-adhesion; secretase; receptor; memory; model; AMYLOID PRECURSOR PROTEIN; HEPARIN-BINDING DOMAIN; GROWTH-FACTOR-I; ALZHEIMERS-DISEASE; OVER-EXPRESSION; CELL-ADHESION; SECRETASE; RECEPTOR; MEMORY; MODEL
ISSN (print) / ISBN 1471-2164
e-ISSN 1471-2164
Zeitschrift BMC Genomics
Quellenangaben Band: 10, Heft: , Seiten: , Artikelnummer: 66 Supplement: ,
Verlag BioMed Central
Begutachtungsstatus Peer reviewed