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Delayed Late Component of Visual Global Field Power in Probable Alzheimer's Disease

Mercer University School of Medicine (Dr Coburn), Macon, GA, the University of California (Dr Ashford), Davis, CA, and the St Francis Hospital (Mr Moreno), Tulsa, OK.

J. Wesson Ashford, MD, PhD

Mercer University School of Medicine (Dr Coburn), Macon, GA, the University of California (Dr Ashford), Davis, CA, and the St Francis Hospital (Mr Moreno), Tulsa, OK.

Marco A. Moreno, BA, R EEG T

Mercer University School of Medicine (Dr Coburn), Macon, GA, the University of California (Dr Ashford), Davis, CA, and the St Francis Hospital (Mr Moreno), Tulsa, OK.

A substantial literature shows that late components of visual evoked potentials (VEPs) are delayed in at least some forms of dementia in the elderly. The late-component delay is selective in that earlier components are not affected. More recent work with better defined clinical groups suggests that the selective late-component delay may be characteristic of Alzheimer's disease (AD) rather than an inevitable feature of dementia in general. To overcome problems in traditional VEP component latency measurement the present study uses reference-free Global Field Power (GFP) analysis to more objectively define VEP components and finds that the GFP peak corresponding to the late P2 component of the flash VEP is delayed in a probable AD group but not in a demented unlikely AD group, relative to age-equivalent healthy controls. The late-component delay is again found to be selective in that the GFP peak corresponding to the earlier PI component of the flash VEP does not differ between groups. These findings further strengthen the evidence for electrocortical changes in the visual system of AD patients.

Journal of Geriatric Psychiatry and Neurology, Vol. 6, No. 2, 72-77 (1993)
DOI: 10.1177/089198879300600203


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