Association between APOE genotype, neuropathology and dementia in the older population of England and Wales
Association between APOE genotype, neuropathology and dementia in the older population of England and Wales
Aims: apolipoprotein E (APOE) genotype is the major genetic risk factor for sporadic Alzheimer's disease (AD) but it is unclear how this is mediated. Most studies of APOE genotype have used case–control design to compare groups differing by two variables: i.e. dementia and AD pathology, so it is unclear to which of these variables APOE genotype is more strongly related. The prospective Medical Research Council Cognitive Function and Ageing Study neuropathology cohort is population-based sample in which donations are unbiased by dementia status.
Methods: we investigated the association between APOE genotypes and neuropathological and cognitive data in this cohort (n = 310).
Results: APOE?4 was associated with an increased risk of diffuse plaques, neuritic plaques, tangles and cerebral amyloid angiopathy. APOE?4 was not associated with infarcts, lacunes, haemorrhages or small vessel disease. APOE?2 appeared to have a protective effect on AD pathology and also on the risk of cortical atrophy. APOE genotype had a non-significant effect on the presence of dementia after adjusting for AD pathology.
Conclusions: APOE genotype is associated with each of the key features of AD pathology but not with cerebrovascular disease other than cerebral amyloid angiopathy. The excess risk of dementia in those with an APOE?4 allele is explained by the pathological features of AD. However, it remains unclear to what extent cognitive dysfunction is caused by these specific pathological features or more directly by closely related APOE-associated mechanisms
285-294
Nicoll, J.A.R.
88c0685f-000e-4eb7-8f72-f36b4985e8ed
Savva, G.M.
3d005012-4857-4c13-aa13-1be1924b5f24
Stewart, J.
856808fb-3362-46ea-b9ed-aa64db4fc983
Matthews, F.E.
66cb45ae-bdc0-4a08-9be6-8f71bb4fff6e
Brayne, C.
b720821a-2b1e-4499-ae06-a26ca10c8a64
Ince, P.
b97c6e4f-a643-41fa-ba4a-e640739fe031
April 2011
Nicoll, J.A.R.
88c0685f-000e-4eb7-8f72-f36b4985e8ed
Savva, G.M.
3d005012-4857-4c13-aa13-1be1924b5f24
Stewart, J.
856808fb-3362-46ea-b9ed-aa64db4fc983
Matthews, F.E.
66cb45ae-bdc0-4a08-9be6-8f71bb4fff6e
Brayne, C.
b720821a-2b1e-4499-ae06-a26ca10c8a64
Ince, P.
b97c6e4f-a643-41fa-ba4a-e640739fe031
Nicoll, J.A.R., Savva, G.M., Stewart, J., Matthews, F.E., Brayne, C. and Ince, P.
(2011)
Association between APOE genotype, neuropathology and dementia in the older population of England and Wales.
Neuropathology and Applied Neurobiology, 37 (3), .
(doi:10.1111/j.1365-2990.2010.01130.x).
(PMID:20880354)
Abstract
Aims: apolipoprotein E (APOE) genotype is the major genetic risk factor for sporadic Alzheimer's disease (AD) but it is unclear how this is mediated. Most studies of APOE genotype have used case–control design to compare groups differing by two variables: i.e. dementia and AD pathology, so it is unclear to which of these variables APOE genotype is more strongly related. The prospective Medical Research Council Cognitive Function and Ageing Study neuropathology cohort is population-based sample in which donations are unbiased by dementia status.
Methods: we investigated the association between APOE genotypes and neuropathological and cognitive data in this cohort (n = 310).
Results: APOE?4 was associated with an increased risk of diffuse plaques, neuritic plaques, tangles and cerebral amyloid angiopathy. APOE?4 was not associated with infarcts, lacunes, haemorrhages or small vessel disease. APOE?2 appeared to have a protective effect on AD pathology and also on the risk of cortical atrophy. APOE genotype had a non-significant effect on the presence of dementia after adjusting for AD pathology.
Conclusions: APOE genotype is associated with each of the key features of AD pathology but not with cerebrovascular disease other than cerebral amyloid angiopathy. The excess risk of dementia in those with an APOE?4 allele is explained by the pathological features of AD. However, it remains unclear to what extent cognitive dysfunction is caused by these specific pathological features or more directly by closely related APOE-associated mechanisms
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Published date: April 2011
Organisations:
Medicine
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Local EPrints ID: 183365
URI: http://eprints.soton.ac.uk/id/eprint/183365
ISSN: 0305-1846
PURE UUID: 70170b69-77fe-46b8-81a2-f28fabc63297
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Date deposited: 03 May 2011 13:29
Last modified: 15 Mar 2024 03:13
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Author:
G.M. Savva
Author:
J. Stewart
Author:
F.E. Matthews
Author:
C. Brayne
Author:
P. Ince
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