Rapid synthesis of internal peptidyl α-ketoamides by on resin oxidation for the construction of rhomboid protease inhibitors

Tim Van Kersavond; Raphael Konopatzki; Merel A T van der Plassche; Jian Yang; Steven H L Verhelst

doi:10.1039/d0ra10614c

Rapid synthesis of internal peptidyl α-ketoamides by on resin oxidation for the construction of rhomboid protease inhibitors

RSC Adv. 2021 Jan 20;11(7):4196-4199. doi: 10.1039/d0ra10614c. eCollection 2021 Jan 19.

Authors

Tim Van Kersavond¹, Raphael Konopatzki¹, Merel A T van der Plassche², Jian Yang², Steven H L Verhelst^{1

2}

Affiliations

¹ Leibniz Institute for Analytical Sciences ISAS e.V., Otto-Hahn-Str. 6b 44227 Dortmund Germany.
² KU Leuven, Department of Cellular and Molecular Medicine, Laboratory of Chemical Biology Herestr. 49 box 802 3000 Leuven Belgium steven.verhelst@kuleuven.be.

Abstract

Rhomboid proteases are intramembrane serine proteases, which are involved in a wide variety of biological processes and have been implied in various human diseases. Recently, peptidyl α-ketoamides have been reported as rhomboid inhibitors with high potency and selectivity - owing to their interaction with both the primed and non-primed site of the target protease. However, their synthesis has been performed by solution phase chemistry. Here, we report a solid phase strategy towards ketoamides as rhomboid protease inhibitors, allowing rapid synthesis and optimization. We found that the primed site binding part of inhibitors is crucial for potency.