Aβ₃₈ in the Brains of Patients with Sporadic and Familial Alzheimer's Disease and Transgenic Mouse Models

Article type: Research Article

Authors: Reinert, Jochim^a | Martens, Henrik^b | Huettenrauch, Melanie^a | Kolbow, Tekla^b | Lannfelt, Lars^c | Ingelsson, Martin^c | Paetau, Anders^d | Verkkoniemi-Ahola, Auli^e | Bayer, Thomas A.^a | Wirths, Oliver^{a; *}

Affiliations: [a] Division of Molecular Psychiatry, Department of Psychiatry, University Medicine Goettingen, Goettingen, Germany | [b] Synaptic Systems GmbH, Goettingen, Germany | [c] Department of Public Health/Geriatrics, Uppsala University, Uppsala, Sweden | [d] Department of Pathology, University and University Hospital of Helsinki, Helsinki, Finland | [e] Department of Neurology, Helsinki University Central Hospital, Helsinki, Finland

Correspondence: [*] Correspondence to: Oliver Wirths, Ph.D., Division of Molecular Psychiatry, Department of Psychiatry, University of Goettingen, von-Siebold-Str. 5, 37075 Goettingen, Germany. Tel.: +49 551 39 10290; Fax: +49 551 39 10291; E-mail: owirths@gwdg.de.

Abstract: The pathogenesis of Alzheimer's disease (AD) is believed to be closely dependent on deposits of neurotoxic amyloid-β peptides (Aβ), which become abundantly present throughout the central nervous system in advanced stages of the disease. The different Aβ peptides existing are generated by subsequent cleavage of the amyloid-β protein precursor (AβPP) and may vary in length and differ at their C-terminus. Despite extensive studies on the most prevalent species Aβ40 and Aβ42, Aβ peptides with other C-termini such as Aβ38 have not received much attention. In the present study, we used a highly specific and sensitive antibody against Aβ38 to analyze the distribution of this Aβ species in cases of sporadic and familial AD, as well as in the brains of a series of established transgenic AD mouse models. We found Aβ38 to be present as vascular deposits in the brains of the majority of sporadic AD cases, whereas it is largely absent in non-demented control cases. Aβ38-positive extracellular plaques were virtually limited to familial cases. Interestingly we observed Aβ38-positive plaques not only among familial cases due to AβPP mutations, but also in cases of familial AD caused by presenilin (PSEN) mutations. Furthermore we demonstrate that Aβ38 deposits in the form of extracellular plaques are common in several AD transgenic mouse models carrying either only AβPP, or combinations of AβPP, PSEN1, and tau transgenes.

Keywords: Aβ₃₈, AβPP, amyloid, mutations, presenilin, transgenic mice, vasculature, vessels

DOI: 10.3233/JAD-131373

Journal: Journal of Alzheimer's Disease, vol. 39, no. 4, pp. 871-881, 2014