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Development of (18)F-Labeled Bispyridyl Tetrazines for In Vivo Pretargeted PET Imaging

Pretargeted PET imaging is an emerging and fast-developing method to monitor immuno-oncology strategies. Currently, tetrazine ligation is considered the most promising bioorthogonal reaction for pretargeting in vivo. Recently, we have developed a method to (18)F-label ultrareactive tetrazines by cop...

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Autores principales: García-Vázquez, Rocío, Jørgensen, Jesper Tranekjær, Bratteby, Klas Erik, Shalgunov, Vladimir, Hvass, Lars, Herth, Matthias M., Kjær, Andreas, Battisti, Umberto Maria
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8879724/
https://www.ncbi.nlm.nih.gov/pubmed/35215356
http://dx.doi.org/10.3390/ph15020245
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author García-Vázquez, Rocío
Jørgensen, Jesper Tranekjær
Bratteby, Klas Erik
Shalgunov, Vladimir
Hvass, Lars
Herth, Matthias M.
Kjær, Andreas
Battisti, Umberto Maria
author_facet García-Vázquez, Rocío
Jørgensen, Jesper Tranekjær
Bratteby, Klas Erik
Shalgunov, Vladimir
Hvass, Lars
Herth, Matthias M.
Kjær, Andreas
Battisti, Umberto Maria
author_sort García-Vázquez, Rocío
collection PubMed
description Pretargeted PET imaging is an emerging and fast-developing method to monitor immuno-oncology strategies. Currently, tetrazine ligation is considered the most promising bioorthogonal reaction for pretargeting in vivo. Recently, we have developed a method to (18)F-label ultrareactive tetrazines by copper-mediated fluorinations. However, bispyridyl tetrazines—one of the most promising structures for in vivo pretargeted applications—were inaccessible using this strategy. We believed that our successful efforts to (18)F-label H-tetrazines using low basic labeling conditions could also be used to label bispyridyl tetrazines via aliphatic nucleophilic substitution. Here, we report the first direct (18)F-labeling of bispyridyl tetrazines, their optimization for in vivo use, as well as their successful application in pretargeted PET imaging. This strategy resulted in the design of [(18)F]45, which could be labeled in a satisfactorily radiochemical yield (RCY = 16%), molar activity (A(m) = 57 GBq/µmol), and high radiochemical purity (RCP > 98%). The [(18)F]45 displayed a target-to-background ratio comparable to previously successfully applied tracers for pretargeted imaging. This study showed that bispyridyl tetrazines can be developed into pretargeted imaging agents. These structures allow an easy chemical modification of (18)F-labeled tetrazines, paving the road toward highly functionalized pretargeting tools. Moreover, bispyridyl tetrazines led to near-instant drug release of iTCO-tetrazine-based ‘click-to-release’ reactions. Consequently, (18)F-labeled bispyridyl tetrazines bear the possibility to quantify such release in vivo in the future.
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spelling pubmed-88797242022-02-26 Development of (18)F-Labeled Bispyridyl Tetrazines for In Vivo Pretargeted PET Imaging García-Vázquez, Rocío Jørgensen, Jesper Tranekjær Bratteby, Klas Erik Shalgunov, Vladimir Hvass, Lars Herth, Matthias M. Kjær, Andreas Battisti, Umberto Maria Pharmaceuticals (Basel) Article Pretargeted PET imaging is an emerging and fast-developing method to monitor immuno-oncology strategies. Currently, tetrazine ligation is considered the most promising bioorthogonal reaction for pretargeting in vivo. Recently, we have developed a method to (18)F-label ultrareactive tetrazines by copper-mediated fluorinations. However, bispyridyl tetrazines—one of the most promising structures for in vivo pretargeted applications—were inaccessible using this strategy. We believed that our successful efforts to (18)F-label H-tetrazines using low basic labeling conditions could also be used to label bispyridyl tetrazines via aliphatic nucleophilic substitution. Here, we report the first direct (18)F-labeling of bispyridyl tetrazines, their optimization for in vivo use, as well as their successful application in pretargeted PET imaging. This strategy resulted in the design of [(18)F]45, which could be labeled in a satisfactorily radiochemical yield (RCY = 16%), molar activity (A(m) = 57 GBq/µmol), and high radiochemical purity (RCP > 98%). The [(18)F]45 displayed a target-to-background ratio comparable to previously successfully applied tracers for pretargeted imaging. This study showed that bispyridyl tetrazines can be developed into pretargeted imaging agents. These structures allow an easy chemical modification of (18)F-labeled tetrazines, paving the road toward highly functionalized pretargeting tools. Moreover, bispyridyl tetrazines led to near-instant drug release of iTCO-tetrazine-based ‘click-to-release’ reactions. Consequently, (18)F-labeled bispyridyl tetrazines bear the possibility to quantify such release in vivo in the future. MDPI 2022-02-18 /pmc/articles/PMC8879724/ /pubmed/35215356 http://dx.doi.org/10.3390/ph15020245 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
García-Vázquez, Rocío
Jørgensen, Jesper Tranekjær
Bratteby, Klas Erik
Shalgunov, Vladimir
Hvass, Lars
Herth, Matthias M.
Kjær, Andreas
Battisti, Umberto Maria
Development of (18)F-Labeled Bispyridyl Tetrazines for In Vivo Pretargeted PET Imaging
title Development of (18)F-Labeled Bispyridyl Tetrazines for In Vivo Pretargeted PET Imaging
title_full Development of (18)F-Labeled Bispyridyl Tetrazines for In Vivo Pretargeted PET Imaging
title_fullStr Development of (18)F-Labeled Bispyridyl Tetrazines for In Vivo Pretargeted PET Imaging
title_full_unstemmed Development of (18)F-Labeled Bispyridyl Tetrazines for In Vivo Pretargeted PET Imaging
title_short Development of (18)F-Labeled Bispyridyl Tetrazines for In Vivo Pretargeted PET Imaging
title_sort development of (18)f-labeled bispyridyl tetrazines for in vivo pretargeted pet imaging
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8879724/
https://www.ncbi.nlm.nih.gov/pubmed/35215356
http://dx.doi.org/10.3390/ph15020245
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