Variability in the type and layer distribution of cortical Aβ pathology in familial Alzheimer's disease

Nanet Willumsen; Teresa Poole; Jennifer M Nicholas; Nick C Fox; Natalie S Ryan; Tammaryn Lashley

doi:10.1111/bpa.13009

Variability in the type and layer distribution of cortical Aβ pathology in familial Alzheimer's disease

Brain Pathol. 2022 May;32(3):e13009. doi: 10.1111/bpa.13009. Epub 2021 Jul 28.

Authors

Nanet Willumsen^{1

2}, Teresa Poole^{3

4}, Jennifer M Nicholas^{3

4}, Nick C Fox^{4

5}, Natalie S Ryan^{4

5}, Tammaryn Lashley^{1

2}

Affiliations

¹ The Queen Square Brain Bank for Neurological Disorders, Department of Clinical and Movement Neurosciences, UCL Queen Square Institute of Neurology, London, UK.
² Department of Neurodegenerative Disease, UCL Queen Square Institute of Neurology, London, UK.
³ Department of Medical Statistics, London School of Hygiene & Tropical Medicine, London, UK.
⁴ Dementia Research Centre, Department of Neurodegenerative Disease, UCL Queen Square Institute of Neurology, London, UK.
⁵ UK Dementia Research Institute at University College London, London, UK.

Abstract

Familial Alzheimer's disease (FAD) is caused by autosomal dominant mutations in the PSEN1, PSEN2 or APP genes, giving rise to considerable clinical and pathological heterogeneity in FAD. Here we investigate variability in clinical data and the type and distribution of Aβ pathologies throughout the cortical layers of different FAD mutation cases. Brain tissue from 20 FAD cases [PSEN1 pre-codon 200 (n = 10), PSEN1 post-codon 200 (n = 6), APP (n = 4)] were investigated. Frontal cortex sections were stained immunohistochemically for Aβ, and Nissl to define the cortical layers. The frequency of different amyloid-beta plaque types was graded for each cortical layer and the severity of cerebral amyloid angiopathy (CAA) was determined in cortical and leptomeningeal blood vessels. Comparisons were made between FAD mutations and APOE4 status, with associations between pathology, clinical and genetic data investigated. In this cohort, possession of an APOE4 allele was associated with increased disease duration but not with age at onset, after adjusting for mutation sub-group and sex. We found Aβ pathology to be heterogeneous between cases although Aβ load was highest in cortical layer 3 for all mutation groups and a higher Aβ load was associated with APOE4. The PSEN1 post-codon 200 group had a higher Aβ load in lower cortical layers, with a small number of this group having increased cotton wool plaque pathology in lower layers. Cotton wool plaque frequency was positively associated with the severity of CAA in the whole cohort and in the PSEN1 post-codon 200 group. Carriers of the same PSEN1 mutation can have differing patterns of Aβ deposition, potentially because of differences in risk factors. Our results highlight possible influences of APOE4 genotype, and PSEN1 mutation type on Aβ deposition, which may have effects on the clinical heterogeneity of FAD.

Keywords: Alzheimer's disease; amyloid; familial Alzheimer’s disease.

Publication types

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

MeSH terms

Alzheimer Disease* / genetics
Alzheimer Disease* / pathology
Amyloid beta-Peptides / genetics
Apolipoprotein E4 / genetics
Cerebral Amyloid Angiopathy* / genetics
Cerebral Amyloid Angiopathy* / pathology
Codon
Humans
Mutation
Plaque, Amyloid / pathology
Presenilin-1 / genetics

Substances

Amyloid beta-Peptides
Apolipoprotein E4
Codon
Presenilin-1

Abstract

Publication types

MeSH terms

Substances

Grants and funding