Abstract
In this study, we have compared the severity of amyloid plaque formation and cerebral amyloid angiopathy (CAA), and the subtype pattern of CAA pathology itself, between APP genetic causes of AD (APPdup, APP mutations), older individuals with Down syndrome (DS) showing the pathology of Alzheimer’s disease (AD) and individuals with sporadic (early and late onset) AD (sEOAD and sLOAD, respectively). The aim of this was to elucidate important group differences and to provide mechanistic insights related to clinical and neuropathological phenotypes. Since lipid and cholesterol metabolism is implicated in AD as well as vascular disease, we additionally aimed to explore the role of APOE genotype in CAA severity and subtypes. Plaque formation was greater in DS and missense APP mutations than in APPdup, sEOAD and sLOAD cases. Conversely, CAA was more severe in APPdup and missense APP mutations, and in DS, compared to sEOAD and sLOAD. When stratified by CAA subtype from 1 to 4, there were no differences in plaque scores between the groups, though in patients with APPdup, APP mutations and sEOAD, types 2 and 3 CAA were more common than type 1. Conversely, in DS, sLOAD and controls, type 1 CAA was more common than types 2 and 3. APOE ε4 allele frequency was greater in sEOAD and sLOAD compared to APPdup, missense APP mutations, DS and controls, and varied between each of the CAA phenotypes with APOE ε4 homozygosity being more commonly associated with type 3 CAA than types 1 and 2 CAA in sLOAD and sEOAD. The differing patterns in CAA within individuals of each group could be a reflection of variations in the efficiency of perivascular drainage, this being less effective in types 2 and 3 CAA leading to a greater burden of CAA in parenchymal arteries and capillaries. Alternatively, as suggested by immunostaining using carboxy-terminal specific antibodies, it may relate to the relative tissue burdens of the two major forms of Aβ, with higher levels of Aβ40 promoting a more ‘aggressive’ form of CAA, and higher levels of Aβ42(3) favouring a greater plaque burden. Possession of APOE ε4 allele, especially ε4 homozygosity, favours development of CAA generally, and as type 3 particularly, in sEOAD and sLOAD.
Highlights
Alzheimer’s disease (AD) is a neurodegenerative disorder characterised clinically by a progressive loss of memory and cognition, accompanied by functional impairments of orientation and praxis
APOE ε4 allele frequency was greater in sEOAD and sLOAD compared to APP duplications (APPdup), missense Amyloid Precursor Protein (APP) mutations, Down syndrome (DS) and controls, and varied between each of the cerebral amyloid angiopathy (CAA) phenotypes with APOE ε4 homozygosity being more commonly associated with type 3 CAA than types 1 and 2 CAA in sLOAD and sEOAD
The severity of CAA was significantly greater in both APPdup (p = 0.005 and p = 0.009, respectively), missense APP mutations (p = 0.016 and p = 0.001, respectively) and DS (p = 0.008 and p < 0.001, respectively) than in sEOAD and sLOAD, and the severity of CAA was greater in APPdup than that in DS (p = 0.014) but not so for missense APP mutations (p = 0.056), with there being no significance difference between the missense APP mutations and DS (Fig. 6b)
Summary
Alzheimer’s disease (AD) is a neurodegenerative disorder characterised clinically by a progressive loss of memory and cognition, accompanied by functional impairments of orientation and praxis. There are rare French [6, 14, 37], Dutch [41], Finnish [38], Japanese [19], Swedish [48] and British [30] families where AD is linked to duplications at the APP locus, resulting in APP overproduction. In most of these families, the duplication has been validated only in living patients and confirmed cases with brain donation are scarce. Recent work suggests that a mutation in the 3′untranslated region of APP result in APP overexpression and might act as a genetic determinant in some cases of CAA [33]
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Disclaimer: All third-party content on this website/platform is and will remain the property of their respective owners and is provided on "as is" basis without any warranties, express or implied. Use of third-party content does not indicate any affiliation, sponsorship with or endorsement by them. Any references to third-party content is to identify the corresponding services and shall be considered fair use under The CopyrightLaw.