The impact of different presenilin 1 and presenilin 2 mutations on amyloid pososition, neurofibrillary changes and neuronal loss in the familial Alzheimer's disease brain. Evidence for other phenotype-modifying factors
ABSTRACT: To assess the influence of the presenilin 1 (PS1) and 2 (PS2) mutations on amyloid deposition, neurofibrillary tangle (NFT) formation and neuronal loss, we performed stereologically based counts in a high-order association cortex, the superior temporal sulcus, of 30 familial Alzheimer'...
- Autores:
-
Gómez Isla, Teresa
Growdon, Whitfield B.
McNamara, Megan J.
Nochlin, David
Bird, Thomas D.
Arango Viana, Juan Carlos
Lopera Restrepo, Francisco Javier
Kosik, Kenneth S.
Lantos, Peter L.
Cairns, Nigel J.
Hyman, Bradley T.
- Tipo de recurso:
- Article of investigation
- Fecha de publicación:
- 1999
- Institución:
- Universidad de Antioquia
- Repositorio:
- Repositorio UdeA
- Idioma:
- eng
- OAI Identifier:
- oai:bibliotecadigital.udea.edu.co:10495/25831
- Acceso en línea:
- http://hdl.handle.net/10495/25831
- Palabra clave:
- Enfermedad de Alzheimer
Alzheimer Disease
Presenilina-1
Presenilin-1
Ovillos Neurofibrilares
Neurofibrillary Tangles
Presenilina-2
Presenilin-2
Aβ plaques
- Rights
- openAccess
- License
- http://creativecommons.org/licenses/by-nc/2.5/co/
| Summary: | ABSTRACT: To assess the influence of the presenilin 1 (PS1) and 2 (PS2) mutations on amyloid deposition, neurofibrillary tangle (NFT) formation and neuronal loss, we performed stereologically based counts in a high-order association cortex, the superior temporal sulcus, of 30 familial Alzheimer's disease cases carrying 10 different PS1 and PS2 mutations, 51 sporadic Alzheimer's disease cases and 33 non-demented control subjects. All the PS1 and PS2 mutations assessed in this series led to enhanced deposition of total Aβ and Aβx-42/43 but not Aβx-40 senile plaques in the superior temporal sulcus when compared with brains from sporadic Alzheimer's disease patients. Some of the PS1 mutations studied (M139V, I143F, G209V, R269H, E280A), but not others, were also associated with faster rates of NFT formation and accelerated neuronal loss in the majority of the patients who harboured them when compared with sporadic Alzheimer's disease patients. In addition, our analysis showed that dramatic quantitative differences in clinical and neuropathological features can exist even among family members with the identical PS mutation. This suggests that further individual or pedigree genetic or epigenetic factors are likely to modulate PS phenotypes strongly. |
|---|