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In vivo quantification of monoamine oxidase A in baboon brain: a PET study using [11C]befloxatone and the multi-injection approach
Authors:Michel Bottlaender   H��ric Valette   Jacques Delforge   Wadad Saba   Ilonka Guenther   Olivier Curet   Pascal George   Fr��d��ric Doll��     Marie-Claude Gr��goire
Affiliation:1CEA, DSV, I2BM, Service Hospitalier Frédéric Joliot, Orsay, France;2Sanofi Aventis Recherche et Développement, Bagneux, France
Abstract:
[11C]befloxatone is a high-affinity, reversible, and selective radioligand for the in vivo visualization of the monoamine oxidase A (MAO-A) binding sites using positron emission tomography (PET). The multi-injection approach was used to study in baboons the interactions between the MAO-A binding sites and [11C]befloxatone. The model included four compartments and seven parameters. The arterial plasma concentration, corrected for metabolites, was used as input function. The experimental protocol—three injections of labeled and/or unlabeled befloxatone—allowed the evaluation of all the model parameters from a single PET experiment. In particular, the brain regional concentrations of the MAO-A binding sites (Bmax) and the apparent in vivo befloxatone affinity (Kd) were estimated in vivo for the first time. A high binding site density was found in almost all the brain structures (170±39 and 194±26 pmol/mL in the frontal cortex and striata, respectively, n=5). The cerebellum presented the lowest binding site density (66±13 pmol/mL). Apparent affinity was found to be similar in all structures (KdVR=6.4±1.5 nmol/L). This study is the first PET-based estimation of the Bmax of an enzyme.
Keywords:[11C]befloxatone   baboon   in vivo   monoamine oxidase A   multi-injection approach   positron emission tomography
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