Alzheimer's Disease Clinical Trial
Official title:
Influence of Age on amyloïd Load in Alzheimer's Disease and in Atypical Focal Cortical Alzheimer's Disease Like Posterior Cortical Atrophy (PCA) and Logopenic Progressive Aphasia (LPA)Using Positron Emitting Tomography (PET) Imaging
The first objective is to asses influence of age on amyloid load measured by PET imaging
using Pittsburgh B compound (PiB) radio-tracer, in Alzheimer's disease(AD). This will allow
the determination of brains age-specific deterioration factors by comparing Early onset AD
(EOAD), Late onset AD (LOAD)and atypical focal cortical AD (PCA and LPA). The amount of
brain lesions in AD patients is estimated by:
1. measuring the rate of cortical brain atrophy,
2. FDG imaging of glucose metabolism reflecting neuronal activity, and
3. for patients who benefited from a lumbar puncture; Cortical-spinal fluid (CSF) amounts
of amyloïd and tau proteins are measured.
Literature data suggests there are different types of AD depending on their age of onset,
called EOAD and LOAD. These two categories are distinguished by the localization of brain
atrophy : severe and 'posterior' in EOAD and more 'anterior' in LOAD. Neuro-pathologic data
suggests some atypical focal cortical atrophy, characterized by a respect of episodic
memory, may be classified within EOAD.
PiB-based PET imaging allows the in-vivo visualization and quantification of amyloïd load.
We want to answer the question whether the amount of amyloïd protein may be lower in LOAD
than EOAD in patients showing the same level of dementia, and thus identify ageing-specific
cognitive disorders and understand witch factors influence etio-pathology of typical and
atypical Alzheimer's disease.
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Observational Model: Case Control, Time Perspective: Prospective
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