Journal of Medicinal Chemistry p. 1593 - 1610 (2021)
Update date:2022-08-29
Topics:
Hoguet, Vanessa
Lasalle, Manuel
Maingot, Mathieu
Dequirez, Geoffroy
Boulahjar, Rajaa
Leroux, Florence
Piveteau, Catherine
Herledan, Adrien
Biela, Alexandre
Dumont, Julie
Chávez-Talavera, Oscar
Belloy, Lo?c
Duplan, Isabelle
Hennuyer, Nathalie
Butruille, Laura
Lestavel, Sophie
Sevin, Emmanuel
Culot, Maxime
Gosselet, Fabien
Staels, Bart
Deprez, Benoit
Tailleux, Anne
Charton, Julie
PEGylation of therapeutic agents is known to improve the pharmacokinetic behavior of macromolecular drugs and nanoparticles. In this work, we performed the conjugation of polyethylene glycols (220-5000 Da) to a series of non-steroidal small agonists of the bile acids receptor TGR5. A suitable anchoring position on the agonist was identified to retain full agonistic potency with the conjugates. We describe herein an extensive structure-properties relationships study allowing us to finely describe the non-linear effects of the PEG length on the physicochemical as well as the in vitro and in vivo pharmacokinetic properties of these compounds. When appending a PEG of suitable length to the TGR5 pharmacophore, we were able to identify either systemic or gut lumen-restricted TGR5 agonists.
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