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Temporal Lobe Atrophy on Magnetic Resonance Imaging in the Diagnosis of Early Alzheimer's Disease
Timo Erkinjuntti, MD, PhD;
Donald H. Lee, MD;
Fuqiang Gao, MD;
Runa Steenhuis, PhD;
Michael Eliasziw, PhD;
Rick Fry;
Harold Merskey, DM;
Vladimir C. Hachinski, MD, DSc(Med)
Arch Neurol. 1993;50(3):305-310.
Abstract
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Objective. —To evaluate the use of simple ratings and linear measures of atrophy in the temporal lobe structures obtained with magnetic resonance imaging coronal scans in the diagnosis of early Alzheimer's disease.
Design. —Prospective series. The National Institute for Neurological Disorders and Stroke—Alzheimer's Disease and Related Disorders Association criteria for probable Alzheimer's disease. Blinded assessment.
Setting. —Dementia study in a university hospital.
Subjects. —Patients with Alzheimer's disease (n=34), scoring 150 or more on the Extended Scale for Dementia, and age-matched healthy community volunteers (n=39) who had both magnetic resonance imaging coronal scans and a psychometric assessment using the Extended Scale for Dementia within 6 months were included.
Measures. —Main measures: T1-weighted magnetic resonance imaging coronal scans, a 1.5-T system. The degree of atrophy rated (0 to 4) in both sides of the temporal neocortex, entorhinal cortex, hippocampal formation, temporal horns, third ventricle, lateral ventricles, and frontal and parietal cortex. Linear measures: the area of hippocampus and the maximal transverse width of temporal horns.
Results. —Differentiation between patients with Alzheimer's disease and controls was limited by considerable variations in sensitivity and specificity. Receiver operating characteristics analysis revealed a clear order of discrimination, the entorhinal cortex and the temporal neocortex being the two best, followed by the temporal horns and hippocampal formation. For a given specificity of 90%, the corresponding sensitivity for the entorhinal cortex, temporal neocortex, temporal horns, and hippocampal formation was 95%, 63%, 56%, and 41 %, respectively. Linear measures differed significantly but showed considerable overlap.
Conclusion. —The presence of rated atrophy in selected temporal structures makes the diagnosis of Alzheimer's disease more likely, but the absence does not rule out the possibility of early Alzheimer's disease.
Author Affiliations
From the Departments of Clinical Neurological Sciences (Drs Erkinjuntti and Hachinski), Neuroradiology (Drs Lee and Gao), and Psychiatry (Mr Fry and Dr Merskey), University of Western Ontario, the Clinical Trials Resources Group (Dr Eliasziw), The John P. Robarts Research Institute (Drs Erkinjuntti, Merskey, and Hachinski), the Department of Psychology, University Hospital (Dr Steenhuis), and The London Psychiatric Hospital (Dr Merskey), London, Ontario; and the Department of Neurology, Memory Research Unit, University of Helsinki (Finland) (Dr Erkinjuntti).
Footnotes
Accepted for publication August 28, 1992.
Reprint requests to Department of Neurology, Memory Research Unit, University of Helsinki, Haartmaninkatu 4, 00290 Helsinki, Finland (Dr Erkinjuntti).
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