Apolipoprotein E isoforms and the development of low and high Braak stages of Alzheimer's disease-related lesions

6533b7d0fe1ef96bd125a571

RESEARCH PRODUCT

Apolipoprotein E isoforms and the development of low and high Braak stages of Alzheimer's disease-related lesions

Thomas G. Ohm Jürgen Bohl Hubert Scharnagl Winfried März

subject

Male Apolipoprotein E medicine.medical_specialty Pathology Genotype Apolipoprotein B Apolipoprotein E2 Apolipoprotein E4 Apolipoprotein E3 tau Proteins Neuropathology Pathology and Forensic Medicine Cellular and Molecular Neuroscience Apolipoproteins E Degenerative disease Isomerism Alzheimer Disease Internal medicine Genotype medicine Humans Allele Alleles Brain Chemistry Amyloid beta-Peptides Polymorphism Genetic biology Brain Neurofibrillary Tangles Neurofibrillary tangle Middle Aged medicine.disease Endocrinology Disease Progression biology.protein Female Neurology (clinical)Alzheimer's disease

description

In recent research, apolipoprotein-E (apoE) polymorphism has been shown to influence the formation of neurofibrillary changes and the accumulation of beta/A4-amyloid, the histopathological hallmarks of Alzheimer's disease (AD). Clinical studies associate the apoE allele epsilon4 with earlier onset of the disease, although the clinical speed of progression remains unchanged. Time course estimates have also provided evidence which indicates that the clinical phase of AD constitutes only 10-20% of the total time span needed for the development of this slowly progressing degenerative brain disorder. Due to the lack of reliable clinical tests for the detection of pre-symptomatic stages of AD, we set out with an autopsy approach to monitor neuropathology of the long pre-clinical phase of AD. This study examined beta/A4-peptide deposition and the formation of neurofibrillary changes staged according to the Braaks' classification in groups of individuals matched for age and sex with different genotypes. In comparison with epsilon3 homozygotes, the presence of the epsilon4 allele is statistically associated with a higher stage of beta/A4-peptide deposition and neurofibrillary change formation (chi2-test, P0.01 for beta/A4-stage and P0.001 for neurofibrillary changes). The effect of the epsilon2 allele differs. Its presence is associated with a lower stage of neurofibrillary pathology in individuals below the age of 80 but with a higher stage thereafter compared to age- and sex-matched epsilon3 homozygotes. Accordingly, the statistical juxtaposition of individuals over 80 years with epsilon4 alleles and those with epsilon2 alleles showed no significant difference with respect to the stages. Our findings indicate that apoE-variants have different effects on the speed of histopathology formation, even in the pre-clinical stages of AD. This suggests that clinical onset, course and pathogenesis of AD are influenced by the apoE genotype.

year	journal	country	edition	language
1999-09-14	Acta Neuropathologica

https://doi.org/10.1007/s004010051080