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Alzheimer's disease clinical variants show distinct neuroinflammatory profiles with neuropathology.

Authors :
Boon, Baayla D. C.
Frigerio, Irene
de Gooijer, Danae
Morrema, Tjado H. J.
Bol, John
Galis ‐ de Graaf, Yvon
Heymans, Martijn
Murray, Melissa E.
van der Lee, Sven J.
Holstege, Henne
van de Berg, Wilma D. J.
Jonkman, Laura E.
Rozemuller, Annemieke J. M.
Bouwman, Femke H.
Hoozemans, Jeroen J. M.
Source :
Neuropathology & Applied Neurobiology; Oct2024, Vol. 50 Issue 5, p1-19, 19p
Publication Year :
2024

Abstract

Aims: Although the neuroanatomical distribution of tau and amyloid‐β is well studied in Alzheimer's disease (AD) (non)‐amnestic clinical variants, that of neuroinflammation remains unexplored. We investigate the neuroanatomical distribution of activated myeloid cells, astrocytes, and complement alongside amyloid‐β and phosphorylated tau in a clinically well‐defined prospectively collected AD cohort. Methods: Clinical variants were diagnosed antemortem, and brain tissue was collected post‐mortem. Typical AD (n = 10), behavioural/dysexecutive AD (n = 6), posterior cortical atrophy (PCA) AD (n = 3), and controls (n = 10) were neuropathologically assessed for AD neuropathology, concurrent pathology including Lewy body disease, limbic‐predominant age‐related TDP‐43 encephalopathy neuropathologic change (LATE‐NC), and vascular pathology. For quantitative assessment, we analysed the corticolimbic distribution of phosphorylated tau, amyloid‐β, CD68, MHC‐II, C4b, and glial fibrillary acidic protein (GFAP) using digital pathology. Results: Phosphorylated tau was distinctly distributed in each variant. In all variants, amyloid‐β was neocortical‐dominant, with a notable increase in the middle frontal cortex of behavioural/dysexecutive AD. Typical AD and PCA AD had no concurrent Lewy body disease, whereas three out of six cases with behavioural/dysexecutive AD did. LATE‐NC stage >0 was observed in three AD cases, two typical AD (stage 1/3), and one behavioural/dysexecutive AD (stage 2/3). Vascular pathology was present in each variant. In typical AD, CD68 and MHC‐II were hippocampal‐dominant. In behavioural/dysexecutive AD, C4b was elevated in the middle frontal and inferior parietal cortex. In PCA AD, MHC‐II was increased in the fusiform gyrus, and GFAP in parietal cortices. Correlations between AD neuropathology and neuroinflammation were distinct within variants. Conclusions: Our data suggests that different involvement of neuroinflammation may add to clinical heterogeneity in AD, which has implications for neuroinflammation‐based biomarkers and future therapeutics. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
03051846
Volume :
50
Issue :
5
Database :
Complementary Index
Journal :
Neuropathology & Applied Neurobiology
Publication Type :
Academic Journal
Accession number :
180520596
Full Text :
https://doi.org/10.1111/nan.13009