In:
Alzheimer's & Dementia, Wiley, Vol. 18, No. S6 ( 2022-12)
Abstract:
Other than the typical (memory‐dominant) variant, Alzheimer’s disease (AD) can present as posterior cortical atrophy (PCA) and behavioral/dysexecutive AD. Tangle distribution differs amongst clinical variants. Neuroinflammation is important in AD pathogenesis and may contribute to Aβ and p‐tau distribution. The relationship between pathological hallmarks, neuroinflammation and, APOE genotype in (a)typical AD is still largely unknown. Method I will discuss our most recent studies on neuroinflammation in (a)typical AD from cohorts derived from the Netherlands Brain Bank and the Mayo Clinic. Atypicality is investigated from both a neuropathological perspective(N=19) and a clinical perspective (N=30, unpublished data). Additionally, the association of APOE ε4 with specific Aβ deposits (i.e., the ‘coarse‐grained plaque’ and the classic cored plaque) and their underlying neuroinflammatory response is investigated (N=60, unpublished data). Result In neuropathologically‐defined atypical AD, microglia, and complement show an atypical distribution across regions, resembling that of p‐tau. Clinical atypical AD variants show in addition to a distinct distribution for p‐tau and Aβ, a distinct distribution for activated microglia (CD68, MHC‐II), complement (C4b), and astrocytes (GFAP) (p 〈 .05) (Fig. 1). Furthermore, when investigating Aβ in detail, we observed an atypical plaque, defined as the ‘coarse‐grained plaque’. This APOE ε4+ plaque is associated with increased neuroinflammation and p‐tau burden (ρ(58)=0.5 and 0.6;p 〈 .05) in contrast to the classic cored plaque. Conclusion Our data supports that not all types of Aβ deposits are associated to p‐tau damage. Neuroinflammation, a process that is differently activated within AD variants, may be the link between Aβ aggregation and subsequent neurodegeneration and contribute to clinical variability.
Type of Medium:
Online Resource
ISSN:
1552-5260
,
1552-5279
Language:
English
Publisher:
Wiley
Publication Date:
2022
detail.hit.zdb_id:
2201940-6
