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000865321 005__ 20210130003015.0
000865321 0247_ $$2doi$$a10.1055/s-0039-1683568
000865321 037__ $$aFZJ-2019-04823
000865321 041__ $$aGerman
000865321 1001_ $$0P:(DE-Juel1)176281$$aCraig, A.$$b0$$eCorresponding author$$ufzj
000865321 1112_ $$a57. Jahrestagung der Deutschen Gesellschaft für Nuklearmedizin$$cBremen$$d2019-04-03 - 2019-04-06$$gNuklearMedizin 2019$$wGermany
000865321 245__ $$aThe Efficient Preparation of Radiolabeled Aromatic Amino Acids via Cu-Mediated Radiofluorination using Ni-complexes
000865321 260__ $$c2019
000865321 3367_ $$033$$2EndNote$$aConference Paper
000865321 3367_ $$2DataCite$$aOther
000865321 3367_ $$2BibTeX$$aINPROCEEDINGS
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000865321 3367_ $$0PUB:(DE-HGF)6$$2PUB:(DE-HGF)$$aConference Presentation$$bconf$$mconf$$s1569411786_25777$$xAfter Call
000865321 520__ $$aZiel/Aim:The aim of this work was to develop a procedure for the preparation of F-18-labeled aromatic amino acids (AAA) via alcohol-enhanced Cu-mediated radiofluorination using Ni-BPX auxiliaries as easily-removable dual-protecting groups.Methodik/Methods:The Bpin-substituted precursors of radiofluorinated AAA and α-Me-AAA were prepared by alkylation of (S)-Ni-BPB-Gly and (S)-Ni-BPA-(RS)-Ala with the corresponding Bpin-substituted benzyl bromides. Radiolabeling was carried out according to the protocol for alcohol-enhanced1 Cu-mediated radiofluorination as follows: F-18-F- was loaded onto a QMA-cartridge which was subsequently washed with MeOH; F-18-F- was eluted with Et4NHCO3 to a solution of Cu(py)4(OTf)2 and precursor in DMF/nBuOH (2:1), and the reaction mixture was stirred under air at 110 °C for 10 min. Evaporation of the DMA/nBuOH was followed by deprotection using 12 M HCl at 110 °C for 15 min. The acidic solution was evaporated and the tracer was isolated by HPLC.Ergebnisse/Results:Ni complexes containing 2 – 4-F-18-FPhe, 2 – 4-aMe-F-18-FPhe, 6-F-18-FMT, aMe-6-F-18-FMT, 4-F-18-FTrp and 2-Me-F-18-FTyr residues were obtained in RCCs of 50 – 95%. The purified tracers were isolated in n.d.c 15 – 25% RCYs in excellent radiochemical and enantiomeric purity. Radiosyntheses of 4-F-18-FPhe and 4-F-18-FTrp were implemented to an automated module furnishing tracers in n.d.c RCYs of 25% and 17%, respectively, within 75 – 80 min.Schlussfolgerungen/Conclusions:Alcohol-enhanced Cu-mediated radiofluorination of BPin substituted Ni-BPX-AAA complexes is a simple, yet powerful method for the fast production of structurally diverse radiolabeled AAAs and alpha-methyl substituted AAAs. The attractiveness of the procedure is highlighted by the accessibility of radiolabeling precursors, high RCYs and easy implementation to an automated module.Literatur/References:[1] Zichler, J., Niklas, K., Modemann, D., Neumaier, B., Zlatopolskiy, B.; Chemistry – A European Journal, 2017, 23, 3251 – 3256
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000865321 7001_ $$0P:(DE-Juel1)178654$$aKolks, N.$$b1$$ufzj
000865321 7001_ $$0P:(DE-Juel1)176705$$aUrusova, E.$$b2$$ufzj
000865321 7001_ $$0P:(DE-Juel1)176188$$aZlatopolskiy, Boris$$b3$$ufzj
000865321 7001_ $$0P:(DE-Juel1)166419$$aNeumaier, B.$$b4$$ufzj
000865321 773__ $$a10.1055/s-0039-1683568
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000865321 9141_ $$y2019
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