Aging Increased Amyloid Peptide and Caused Amyloid Plaques in Brain of Old APP/V717I Transgenic Mice by a Different Mechanism than Mutant Presenilin1

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The Journal of Neuroscience, September 1, 2000, 20(17):6452-6458

Aging Increased Amyloid Peptide and Caused Amyloid Plaques in Brain of Old APP/V717I Transgenic Mice by a Different Mechanism than Mutant Presenilin1
Ilse Dewachter¹, Jo Van Dorpe¹, Liesbet Smeijers¹, Martine Gilis¹, Cuno Kuipéri¹, Isabelle Laenen¹, Nathalie Caluwaerts¹, Dieder Moechars⁴, Frédéric Checler², Hugo Vanderstichele³, and Fred Van Leuven¹
¹ Experimental Genetics Group, Center for Human Genetics, Flemish Institute for Biotechnology, Katholieke Universiteit Leuven, B-3000 Leuven, Belgium, ² Institut de Pharmacologie Moléculaire et Cellulaire/Centre National de la Recherche Scientifique, Unité Propre de Recherche 411, Valbonne 06560, France, ³ Innogenetics NV, Industriepark Zwijnaarde, 9052 Gent, Belgium, and ⁴ Janssen Research Foundation, 2340 Beerse, Belgium
Aging of transgenic mice that overexpress the London mutant of amyloid precursor protein (APP/V717I) (Moechars et al., 1999a)was now demonstrated not to affect the normalized levels of $alpha$ -or $beta$ -cleaved secreted APP nor of the $beta$ -C-terminal stubs. Thisindicated that aging did not markedly disturb either $alpha$ - or $beta$ -secretasecleavage of APP and failed to explain the origin of the massiveamounts of amyloid peptides A $beta$ 40 and A $beta$ 42, soluble and precipitatedas amyloid plaques in the brain of old APP/V717I transgenic mice.We tested the hypothesis that aging acted on presenilin1 (PS1)to affect $gamma$ -secretase-mediated production of amyloid peptidesby comparing aged APP/V717I transgenic mice to double transgenicmice coexpressing human PS1 and APP/V717I. In double transgenicmice with mutant (A246E) but not wild-type human PS1, brain amyloidpeptide levels increased and resulted in amyloid plaques whenthe mice were only 6-9 months old, much earlier than in APP/V717Itransgenic mice (12-15 months old). Mutant PS1 increased mainlybrain A $beta$ 42 levels, whereas in aged APP/V717I transgenic mice,both A $beta$ 42 and A $beta$ 40 increased. This resulted in a dramatic differencein the A $beta$ 42/A $beta$ 40 ratio of precipitated or plaque-associated amyloidpeptides, i.e., 3.11 ± 0.22 in double APP/V717I × PS1/A246E transgenicmice compared with 0.43 ± 0.07 in aged APP/V717I transgenic mice,and demonstrated a clear difference between the effect of agingand the effect of the insertion of a mutant PS1 transgene. Inconclusion, we demonstrate that aging did not favor amyloidogenicover nonamyloidogenic processing of APP, nor did it exert a mutantPS1-like effect on $gamma$ -secretase. Therefore, the data are interpretedto suggest that parenchymal and vascular accumulation of amyloidin aging brain resulted from failure to clear the amyloid peptidesrather than from increasedproduction.

Key words: amyloid precursor protein; APP processing; aging; presenilin; transgenic mice; amyloid plaques; amyloid peptide
Copyright © 2000 Society for Neuroscience 0270-6474/00/20176452-07$05.00/0

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