In Vitro Evaluation of 11C-Labeled (S)-Nicotine, (S)-3-Methyl-5-(1-Methyl-2-Pyrrolidinyl)isoxazole, and (R,S)-1-Methyl-2-(3-Pyridyl)azetidine as Nicotinic Receptor Ligands for Positron Emission Tomography Studies |
| |
| Authors: | †Wiebke Sihver Karl-Johan Fasth Mattias Ögren ‡Håkan Bivehed Mats Bergström §Agneta Nordberg †&#;Yasuyoshi Watanabe Bengt Långström |
| |
| Institution: | Subfemtomole Biorecognition Project, Japan Science and Technology Corporation and PET Centre;; Department of Medical Pharmacology, Uppsala University, Uppsala;; Swedish Match, Research &Analysis, Stockholm;; Karolinska Institute, Department of Clinical Neuroscience and Family Medicine, Division of Molecular Neuropharmacology, Huddinge Hospital, Huddinge, Sweden;and; Osaka Bioscience Institute, Osaka, Japan |
| |
| Abstract: | Abstract: The binding characteristics of the novel 11C-labeled nicotinic ligands (R,S)-1-methyl-2-(3-pyridyl) azetidine (MPA) and (S)-3-methyl-5-(1-methyl-2-pyrrolidinyl)isoxazole (ABT-418) were investigated in comparison with those of (S)-11C]nicotine in vitro in the rat brain to be able to predict the binding properties of the new ligands for positron emission tomography studies in vivo. The data from time-resolved experiments for all ligands indicated fast binding kinetics, with the exception of a slower dissociation of 11C]MPA in comparison with (S)-11C]nicotine and 11C]ABT-418. Saturation experiments revealed for all ligands two nicotinic receptor binding sites with affinity constants (KD values) of 2.4 and 560 nM and binding site densities (Bmax values) of 65.5 and 223 fmol/mg of protein for (S)-11C]nicotine, KD values of 0.011 and 2.2 nM and Bmax values of 4.4 and 70.7 fmol/mg of protein for 11C]MPA, and KD values of 1.3 and 33.4 nM and Bmax values of 8.8 and 69.2 fmol/mg of protein for 11C]ABT-418. In competing with the 11C-ligands, epibatidine was most potent, followed by cytisine. A different rank order of potencies was found for (?)-nicotine, (+)-nicotine, MPA, and ABT-418 displacing each of the 11C-ligands. Autoradiograms displayed a similar pattern of receptor binding for all ligands, whereby 11C]MPA showed the most distinct binding pattern and the lowest nonspecific binding. We conclude that the three 11C-labeled nicotinic ligands were suitable for characterizing nicotinic receptors in vitro. The very high affinity of 11C]MPA to nicotinic acetylcholine receptors, its low nonspecific binding, and especially the slower dissociation kinetics of the 11C]MPA from the putative high-affinity nicotinic acetylcholine receptor binding site compared with (S)-11C]nicotine and 11C]ABT-418 raise the level of interest in 11C]MPA for application in positron emission tomography. |
| |
| Keywords: | Nicotinic receptor Positron emission tomography (R S)-1-[11C]Methyl-2-(3-pyridyl)-azetidine (S) - 3 - Methyl - 5 - (1 - [11C]methyl - 2 - pyrrolidinyl)isoxazole (S)-[11C]Nicotine In vitro receptor binding |
|
|
