[(18)F]Fluorophenylazocarboxylates: Design and Synthesis of Potential Radioligands for Dopamine D3 and μ-Opioid Receptor

[Image: see text] (18)F-Labeled building blocks from the type of [(18)F]fluorophenylazocarboxylic-tert-butyl esters offer a rapid, mild, and reliable method for the (18)F-fluoroarylation of biomolecules. Two series of azocarboxamides were synthesized as potential radioligands for dopamine D3 and the...

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Autores principales: Nebel, Natascha, Strauch, Brigitte, Maschauer, Simone, Lasch, Roman, Rampp, Hannelore, Fehler, Stefanie K., Bock, Leonard R., Hübner, Harald, Gmeiner, Peter, Heinrich, Markus R., Prante, Olaf
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2017
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5819854/
https://www.ncbi.nlm.nih.gov/pubmed/29479577
http://dx.doi.org/10.1021/acsomega.7b01374
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author Nebel, Natascha
Strauch, Brigitte
Maschauer, Simone
Lasch, Roman
Rampp, Hannelore
Fehler, Stefanie K.
Bock, Leonard R.
Hübner, Harald
Gmeiner, Peter
Heinrich, Markus R.
Prante, Olaf
author_facet Nebel, Natascha
Strauch, Brigitte
Maschauer, Simone
Lasch, Roman
Rampp, Hannelore
Fehler, Stefanie K.
Bock, Leonard R.
Hübner, Harald
Gmeiner, Peter
Heinrich, Markus R.
Prante, Olaf
author_sort Nebel, Natascha
collection PubMed
description [Image: see text] (18)F-Labeled building blocks from the type of [(18)F]fluorophenylazocarboxylic-tert-butyl esters offer a rapid, mild, and reliable method for the (18)F-fluoroarylation of biomolecules. Two series of azocarboxamides were synthesized as potential radioligands for dopamine D3 and the μ-opioid receptor, revealing compounds 3d and 3e with single-digit and sub-nanomolar affinity for the D3 receptor and compound 4c with only micromolar affinity for the μ-opioid receptor, but enhanced selectivity for the μ-subtype in comparison to the lead compound AH-7921. A “minimalist procedure” without the use of a cryptand and base for the preparation of 4-[(18)F]fluorophenylazocarboxylic-tert-butyl ester [(18)F]2a was established, together with the radiosynthesis of methyl-, methoxy-, and phenyl-substituted derivatives ([(18)F]2b–f). With the substituted [(18)F]fluorophenylazocarbylates in hand, two prototype azocarboxylates radioligands were synthesized by (18)F-fluoroarylation, namely the methoxy azocarboxamide [(18)F]3d as the D3 receptor radioligand and [(18)F]4a as a prototype structure of the μ-opioid receptor radioligand. By introducing the new series of [(18)F]fluorophenylazocarboxylic-tert-butyl esters, the method of (18)F-fluoroarylation was significantly expanded, thereby demonstrating the versatility of (18)F-labeled phenylazocarboxylates for the design of potential radiotracers for positron emission tomography .
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spelling pubmed-58198542018-02-21 [(18)F]Fluorophenylazocarboxylates: Design and Synthesis of Potential Radioligands for Dopamine D3 and μ-Opioid Receptor Nebel, Natascha Strauch, Brigitte Maschauer, Simone Lasch, Roman Rampp, Hannelore Fehler, Stefanie K. Bock, Leonard R. Hübner, Harald Gmeiner, Peter Heinrich, Markus R. Prante, Olaf ACS Omega [Image: see text] (18)F-Labeled building blocks from the type of [(18)F]fluorophenylazocarboxylic-tert-butyl esters offer a rapid, mild, and reliable method for the (18)F-fluoroarylation of biomolecules. Two series of azocarboxamides were synthesized as potential radioligands for dopamine D3 and the μ-opioid receptor, revealing compounds 3d and 3e with single-digit and sub-nanomolar affinity for the D3 receptor and compound 4c with only micromolar affinity for the μ-opioid receptor, but enhanced selectivity for the μ-subtype in comparison to the lead compound AH-7921. A “minimalist procedure” without the use of a cryptand and base for the preparation of 4-[(18)F]fluorophenylazocarboxylic-tert-butyl ester [(18)F]2a was established, together with the radiosynthesis of methyl-, methoxy-, and phenyl-substituted derivatives ([(18)F]2b–f). With the substituted [(18)F]fluorophenylazocarbylates in hand, two prototype azocarboxylates radioligands were synthesized by (18)F-fluoroarylation, namely the methoxy azocarboxamide [(18)F]3d as the D3 receptor radioligand and [(18)F]4a as a prototype structure of the μ-opioid receptor radioligand. By introducing the new series of [(18)F]fluorophenylazocarboxylic-tert-butyl esters, the method of (18)F-fluoroarylation was significantly expanded, thereby demonstrating the versatility of (18)F-labeled phenylazocarboxylates for the design of potential radiotracers for positron emission tomography . American Chemical Society 2017-12-06 /pmc/articles/PMC5819854/ /pubmed/29479577 http://dx.doi.org/10.1021/acsomega.7b01374 Text en Copyright © 2017 American Chemical Society This is an open access article published under an ACS AuthorChoice License (http://pubs.acs.org/page/policy/authorchoice_termsofuse.html) , which permits copying and redistribution of the article or any adaptations for non-commercial purposes.
spellingShingle Nebel, Natascha
Strauch, Brigitte
Maschauer, Simone
Lasch, Roman
Rampp, Hannelore
Fehler, Stefanie K.
Bock, Leonard R.
Hübner, Harald
Gmeiner, Peter
Heinrich, Markus R.
Prante, Olaf
[(18)F]Fluorophenylazocarboxylates: Design and Synthesis of Potential Radioligands for Dopamine D3 and μ-Opioid Receptor
title [(18)F]Fluorophenylazocarboxylates: Design and Synthesis of Potential Radioligands for Dopamine D3 and μ-Opioid Receptor
title_full [(18)F]Fluorophenylazocarboxylates: Design and Synthesis of Potential Radioligands for Dopamine D3 and μ-Opioid Receptor
title_fullStr [(18)F]Fluorophenylazocarboxylates: Design and Synthesis of Potential Radioligands for Dopamine D3 and μ-Opioid Receptor
title_full_unstemmed [(18)F]Fluorophenylazocarboxylates: Design and Synthesis of Potential Radioligands for Dopamine D3 and μ-Opioid Receptor
title_short [(18)F]Fluorophenylazocarboxylates: Design and Synthesis of Potential Radioligands for Dopamine D3 and μ-Opioid Receptor
title_sort [(18)f]fluorophenylazocarboxylates: design and synthesis of potential radioligands for dopamine d3 and μ-opioid receptor
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5819854/
https://www.ncbi.nlm.nih.gov/pubmed/29479577
http://dx.doi.org/10.1021/acsomega.7b01374
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