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Parametric in vivo imaging of benzodiazepine receptor distribution in human brain.

作者信息

Frey K A, Holthoff V A, Koeppe R A, Jewett D M, Kilbourn M R, Kuhl D E

机构信息

Division of Nuclear Medicine (Department of Internal Medicine) University of Michigan, Ann Arbor.

出版信息

Ann Neurol. 1991 Nov;30(5):663-72. doi: 10.1002/ana.410300506.

DOI:10.1002/ana.410300506
PMID:1662476
Abstract

Emission computed tomographic methods for the in vivo quantification of radioligand-binding sites in human brain have previously been limited either by a lack of correction for possible effects of altered ligand transport or by highly complicated physiological models that preclude display of binding data in a detailed anatomical format. We investigated the application of a simplified compartmental model to the kinetic analysis of in vivo ligand binding to central benzodiazepine receptors. The human brain distribution of [11C]flumazenil, as determined by dynamic positron emission tomography, combined with metabolite-corrected arterial blood samples, permitted estimations of local cerebral ligand transport and of receptor binding. This approach allows calculation of transport and binding "maps" on a pixel-by-pixel basis, resulting in the display of binding data in a familiar tomographic format while maintaining much of the physiological accuracy inherent in more complex methods. The results obtained in a study of 6 normal volunteers revealed good interindividual precision, with coefficients of variation between 10 and 15% of mean regional values, suggesting the utility of this approach in future clinical studies of benzodiazepine receptor binding.

摘要

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