Accumulation of murine amyloid-β mimics early Alzheimer's disease

Markus Krohn; Alexander Bracke; Yosef Avchalumov; Toni Schumacher; Jacqueline Hofrichter; Kristin Paarmann; Christina Fröhlich; Cathleen Lange; Thomas Brüning; Oliver von Bohlen Und Halbach; Jens Pahnke

doi:10.1093/brain/awv137

Accumulation of murine amyloid-β mimics early Alzheimer's disease

Brain. 2015 Aug;138(Pt 8):2370-82. doi: 10.1093/brain/awv137. Epub 2015 May 18.

Affiliations

¹ 1 Translational Neurodegeneration Research and Neuropathology Lab, Department of Neuro-/Pathology, University of Oslo (UiO) and Oslo University Hospital (OUS), Oslo, Norway 2 Department of Neurology, University of Rostock, Rostock, Germany.
² 3 Department of Anatomy, University of Greifswald, Greifswald, Germany.
³ 4 Department of Physiology, University of Rostock, Rostock, Germany.
⁴ 2 Department of Neurology, University of Rostock, Rostock, Germany.
⁵ 1 Translational Neurodegeneration Research and Neuropathology Lab, Department of Neuro-/Pathology, University of Oslo (UiO) and Oslo University Hospital (OUS), Oslo, Norway 2 Department of Neurology, University of Rostock, Rostock, Germany 5 University of Lübeck, LIED, Lübeck, Germany 6 Department of Bioorganic Chemistry, Leibniz Institute of Plant Biochemistry, Halle, Germany jens.pahnke@medisin.uio.no.

PMID: 25991605
DOI: 10.1093/brain/awv137

Abstract

Amyloidosis mouse models of Alzheimer's disease are generally established by transgenic approaches leading to an overexpression of mutated human genes that are known to be involved in the generation of amyloid-β in Alzheimer's families. Although these models made substantial contributions to the current knowledge about the 'amyloid hypothesis' of Alzheimer's disease, the overproduction of amyloid-β peptides mimics only inherited (familiar) Alzheimer's disease, which accounts for <1% of all patients with Alzheimer's disease. The inherited form is even regarded a 'rare' disease according to the regulations for funding of the European Union (www.erare.eu). Here, we show that mice that are double-deficient for neprilysin (encoded by Mme), one major amyloid-β-degrading enzyme, and the ABC transporter ABCC1, a major contributor to amyloid-β clearance from the brain, develop various aspects of sporadic Alzheimer's disease mimicking the clinical stage of mild cognitive impairment. Using behavioural tests, electrophysiology and morphological analyses, we compared different ABC transporter-deficient animals and found that alterations are most prominent in neprilysin × ABCC1 double-deficient mice. We show that these mice have a reduced probability to survive, show increased anxiety in new environments, and have a reduced working memory performance. Furthermore, we detected morphological changes in the hippocampus and amygdala, e.g. astrogliosis and reduced numbers of synapses, leading to defective long-term potentiation in functional measurements. Compared to human, murine amyloid-β is poorly aggregating, due to changes in three amino acids at N-terminal positions 5, 10, and 13. Interestingly, our findings account for the action of early occurring amyloid-β species/aggregates, i.e. monomers and small amyloid-β oligomers. Thus, neprilysin × ABCC1 double-deficient mice present a new model for early effects of amyloid-β-related mild cognitive impairment that allows investigations without artificial overexpression of inherited Alzheimer's disease genes.

Keywords: ABCB1; ABCC1; Alzheimer’s disease; MCI; amyloidosis; neprilysin.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Alzheimer Disease / genetics*
Alzheimer Disease / metabolism
Amyloid beta-Peptides / metabolism*
Animals
Cognitive Dysfunction / genetics
Disease Models, Animal
Hippocampus / metabolism*
Long-Term Potentiation
Mice, Knockout
Multidrug Resistance-Associated Proteins / genetics*
Neprilysin / genetics*
Neprilysin / metabolism
Neurons / metabolism

Substances

Amyloid beta-Peptides
Multidrug Resistance-Associated Proteins
Neprilysin
multidrug resistance-associated protein 1