Efficient palladium-catalyzed electrocarboxylation enables late-stage carbon isotope labelling.

Nat Commun

Carbon Dioxide Activation Center (CADIAC), Novo Nordisk Foundation CO2 Research Center, Interdisciplinary Nanoscience Center, Department of Chemistry, Aarhus University, Gustav Wieds Vej 14, Aarhus C, Denmark.

Published: March 2024

AI Article Synopsis

  • Carbon isotope labeling is crucial for understanding how new drugs work in the body, particularly their pharmacokinetic and pharmacodynamic properties.
  • Aryl carboxylic acids are common in drugs and can be labeled using isotopically labeled carbon monoxide, but traditional methods have limitations due to excess CO and catalyst issues.
  • The study introduces a new, cost-effective method using a palladium-catalyzed electrocarboxylation technique that allows for more efficient carbon-14 labeling of pharmaceuticals, enhancing drug development.

Article Abstract

Carbon isotope labelling of bioactive molecules is essential for accessing the pharmacokinetic and pharmacodynamic properties of new drug entities. Aryl carboxylic acids represent an important class of structural motifs ubiquitous in pharmaceutically active molecules and are ideal targets for the installation of a radioactive tag employing isotopically labelled CO. However, direct isotope incorporation via the reported catalytic reductive carboxylation (CRC) of aryl electrophiles relies on excess CO, which is incompatible with carbon-14 isotope incorporation. Furthermore, the application of some CRC reactions for late-stage carboxylation is limited because of the low tolerance of molecular complexity by the catalysts. Herein, we report the development of a practical and affordable Pd-catalysed electrocarboxylation setup. This approach enables the use of near-stoichiometric CO generated from the primary carbon-14 source BaCO, facilitating late-stage and single-step carbon-14 labelling of pharmaceuticals and representative precursors. The proposed isotope-labelling protocol holds significant promise for immediate impact on drug development programmes.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10959938PMC
http://dx.doi.org/10.1038/s41467-024-46820-9DOI Listing

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