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@INPROCEEDINGS{Drerup:825272,
author = {Drerup, Christian and Brandt, Marie and Ermert, Johannes
and Coenen, Heinrich Hubert},
title = {{S}ynthesis of an {F}-18-labelled {NO}-synthase inhibitor},
reportid = {FZJ-2016-07743},
year = {2015},
abstract = {Objectives: Nitric oxide (NO), an important signalling
molecule in the human body, is synthesised by three isoforms
of NO-synthase (NOS) from the amino acid L-arginine.
Overproduction of NO by neuronal NOS has been associated
with neurodegenerative disorders. Therefore, developing
small molecules for selective inhibition of nNOS over
related isoforms (iNOS and eNOS) is therapeutically
desirable and of great interest for decoding
neurodestructive key factors [1]. Suitable 18F-labelled
NOS-Inhibitors should allow the investigation of
NOS-function by molecular imaging. Potentially, the highly
selective nNOS Inhibitor
6-((3-((3-fluorophenylethylamino)methyl)phenoxy)methyl)-4-methyl-pyridine-2-amine
[2] is a suitable target for labelling with n.c.a.
[18F]fluoride in addition to the established iNOS inhibitor
6-(2-[18F]fluoropropyl)-4-methylpyridine-2-amine
[3].Methods: Based on
tert-butyl-(3-iodophenylethyl)carbamate the corresponding
iodoniumylide precursor was formed [4]. The activated
aromatic system was labelled with n.c.a. [18F]fluoride and
converted via reductive amination followed by microwave
assisted displacement of the protecting groups to the
desired nNOS inhibitor. For the development of a simplified
late-stage labelling procedure the corresponding brominated,
Boc- and pyrrole-protected compound was synthesised, which
was converted via borylation into the boronic ester
precursor. This compound was labelled authentically by
copper(II) mediated n.c.a. 18F-fluorination [5]. Further
developments enabled the one-pot synthesis by adapting the
[18F]fluoride activation to the radiolabelling step leading
to ready-to-automate conditions. Furthermore, an automated
one-pot procedure for the synthesis of the iNOS-Inhibitor
was examined after stability tests and kinetic
studies.Results: The n.c.a. 18F-fluorination of the
iodoniumylide precursor proceeded efficiently and
regioselective in 79 $\%$ radiochemical yield (RCY). The
following built-up synthesis led to the desired nNOS
inhibitor in 15 $\%$ RCY. First attempts of the late-stage
copper(II) mediated n.c.a. 18F-fluorination led to similar
conversions. The labelling procedure was reduced to a
simplified one-pot synthesis. Conclusion: Finally, there are
now potential and isoform selective radiotracers for both
inducible and neuronal NO-synthases with high molar
activities for further evaluations and preclinical
studies.References: [1] Mukherjee P. et al. (2014), Chem.
Soc. Rev., 43, 6814-6838.[2] Jing Q. et al. (2013), Bioorg.
Med. Chem., 21, 5323. [3] Zhou D. et al. (2009), J. Med.
Chem., 52, 2443.[4] Cardinale J. et al. (2013), Tetr. Lett.,
54, 2067.[5] Tredwell M. et al. (2014), Angew. Chem. Int.
Ed., 53, 7751.},
month = {May},
date = {2015-05-26},
organization = {21st International Symposium on
Radiopharmaceutical Sciences, Columbia
(USA), 26 May 2015 - 31 May 2015},
subtyp = {Plenary/Keynote},
cin = {INM-5},
cid = {I:(DE-Juel1)INM-5-20090406},
pnm = {573 - Neuroimaging (POF3-573)},
pid = {G:(DE-HGF)POF3-573},
typ = {PUB:(DE-HGF)6},
url = {https://juser.fz-juelich.de/record/825272},
}
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