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Assessment of labelled products with different radioanalytical methods: study on 18F-fluorination reaction of 4-[18F]fluoro-N-[2-[1-(2-methoxyphenyl)-1-piperazinyl]ethyl-N-2-pyridinyl-benzamide (p-[18F]MPPF)
Authors:Teija Koivula  Jaana Laine  Tiina Lipponen  Outi Perhola  Eeva-Liisa K?m?r?inen  Kim Bergstr?m and Olof Solin
Institution:(1) Laboratory of Radiochemistry, University of Helsinki, PO Box 55, 00014 Helsinki, Finland;(2) Laboratory of Analytical Chemistry, University of Helsinki, PO Box 55, 00014 Helsinki, Finland;(3) Division of Nuclear Medicine, Helsinki University Central Hospital, PO Box 340, 00029 Helsinki, Finland;(4) Imanext Ltd, PO Box 800, 00101 Helsinki, Finland;(5) Centre for Drug Research, Faculty of Pharmacy, University of Helsinki, PO Box 56, 00014 Helsinki, Finland;(6) Radiopharmaceutical Chemistry Laboratory, Turku PET Centre, Porthaninkatu 3, 20500 Turku, Finland
Abstract:The serotonin receptor 5-HT1A ligand 4-18F]fluoro-N-2-1-(2-methoxyphenyl)-1-piperazinyl]ethyl-N-2-pyridinyl-benzamide (p-18F]MPPF) was produced by a simplified method of Le Bars et al. Traditional oil bath heating was compared to microwave heating. Various radioanalytical methods, radio-Thin Layer Chromatography (TLC), High Pressure Liquid Chromatography (HPLC) and Mass Spectrometry (MS), were compared in the evaluation of the labelled product(s). The crude reaction mixture consisted of p-18F]MPPF and 2–4 radioactive by-products eluting after the product fraction, and the reverse-phase HPLC method failed occasionally to separate p-18F]MPPF from the radioactive by-product with close retention time. The heating method had no significant effect on the composition of labelled by-products. In LC-(ESI)-MS analysis of p-18F]MPPF the labelled product was identified with m/z ratio of 435 (M + H+]). The other HPLC fractions were measured to have following m/z ratios: (1) 327; 349; (675) (2) 402; 407/408; (791) and (3) 436, suggesting different kind of decomposition of the labelled product and/or the inactive precursor. The ion trap mass spectrometer was sufficient for the qualitative analysis of p-18F]MPPF. However, differentiation of by-products arising from the decomposition of p-18F]MPPF or from its precursor p-MPPNO2 proved to be challenging.
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