Kinase inhibition by deoxy analogues of the resorcylic lactone L-783277

Marc Liniger; Christian Neuhaus; Tatjana Hofmann; Luca Fransioli-Ignazio; Michel Jordi; Peter Drueckes; Jörg Trappe; Doriano Fabbro; Karl-Heinz Altmann

doi:10.1021/ml1001807

Kinase inhibition by deoxy analogues of the resorcylic lactone L-783277

ACS Med Chem Lett. 2010 Oct 20;2(1):22-7. doi: 10.1021/ml1001807. eCollection 2011 Jan 13.

Authors

Marc Liniger¹, Christian Neuhaus¹, Tatjana Hofmann¹, Luca Fransioli-Ignazio¹, Michel Jordi¹, Peter Drueckes², Jörg Trappe², Doriano Fabbro², Karl-Heinz Altmann¹

Affiliations

¹ Swiss Federal Institute of Technology (ETH) Zurich, Department of Chemistry and Applied Biosciences, Institute of Pharmaceutical Sciences, 8093 Zurich, Switzerland.
² Novartis Institute for Biomedical Research, Center for Proteomic Chemistry, Expertise Platform Kinases, 4002 Basel, Switzerland.

Abstract

The natural product L-783277 is a resorcylic lactone type covalent kinase inhibitor. We have prepared the 5'-deoxy analogue of L-783277 (1) in a stereoselective fashion. Remarkably, this analogue retains almost the full kinase inhibitory potential of natural L-783277, with low nanomolar IC50 values against the most sensitive kinases, and it exhibits essentially the same selectivity profile (within the panel of 39 kinases investigated). In contrast, removal of both the 4'- and the 5'-hydroxyl groups leads to a more significant reduction in kinase inhibitory activity and so does a change in the geometry of the C7'-C8' double bond in 1 from Z to E. These findings offer new perspectives for the design of second generation resorcylic lactone-based kinase inhibitors.

Keywords: Cancer; SAR; irreversible inhibitor; kinase inhibitor; natural product; resorcylic lactone (RL); stereoselective synthesis.