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ORIGINAL ARTICLE
The Quarterly Journal of Nuclear Medicine and Molecular Imaging 2022 June;66(2):148-55
DOI: 10.23736/S1824-4785.19.03175-3
Copyright © 2019 EDIZIONI MINERVA MEDICA
lingua: Inglese
Imaging of dopamine transporter with [18F]LBT-999: initial evaluation in healthy volunteers
Nicolas ARLICOT 1, 2, 3 ✉, Johnny VERCOUILLIE 2, 3, Cécile MALHERBE 1, 2, Rudy BIDAULT 2, Valérie GISSOT 3, Serge MAIA 1, 2, Laurent BARANTIN 2, Jean-Philippe COTTIER 2, 4, Jean-Bernard DELOYE 5, Denis GUILLOTEAU 2, 3 6, Maria-Joao RIBEIRO 2, 3, 7
1 CHRU de Tours, Unit of Radiopharmacy, Tours, France; 2 UMR 1253, iBrain, University of Tours, Tours, France; 3 INSERM CIC 1415, University Hospital of Tours, Tours, France; 4 CHRU de Tours, Department of Neuroradiology, Tours, France; 5 Zionexa, Paris, France; 6 CHRU de Tours, Department of In Vitro Nuclear Medicine, Tours, France; 7 CHRU de Tours, Department of In Vivo Nuclear Medicine, Tours, France
BACKGROUND: The aim of this study was to evaluate in healthy human brain the distribution, uptake, and kinetics of [18F]LBT-999, a PET ligand targeting the dopamine transporter, to assess its ability to explore dopaminergic innervation, using a shorter protocol, more convenient for patients than currently with [123I]ioflupane.
METHODS: After intravenous injection of [18F]LBT-999, 8 healthy subjects (53-80y) underwent a dynamic PET-scan. Venous samples were concomitantly obtained for metabolites analysis. Time activity curves (TACs) were generated for several ROIs (caudate, putamen, occipital cortex, substantia nigra and cerebellum). Cerebellum was used as reference region to calculate binding potentials (BP
RESULTS: No adverse events or detectable pharmacological effects were reported. [18F]LBT-999 PET revealed a good cerebral distribution, with an intense and symmetric uptake in both putamen and caudate (BP
CONCLUSIONS: These findings support the usefulness of [18F]LBT-999 for a quantitative clinical evaluation of presynaptic dopaminergic innervation.
KEY WORDS: Radiopharmaceuticals; Positron-emission tomography; Dopamine plasma membrane transport proteins; Parkinson disease