Isosteric replacements for benzothiazoles and optimisation to potent Cathepsin K inhibitors free from hERG channel inhibition

Article ID	Journal	Published Year	Pages	File Type
10594616	Bioorganic & Medicinal Chemistry Letters	2012	6 Pages	PDF

Abstract

The discovery of nitrile compound 4, a potent inhibitor of Cathepsin K (Cat K) with good bio-availability in dog is described. The compound was used to demonstrate target engagement and inhibition of Cat K in an in vivo dog PD model. The margin to hERG ion channel inhibition was deemed too low for a clinical candidate and an optimisation program to find isosteres or substitutions on benzothiazole group led to the discovery of 20, 24 and 27; all three free from hERG inhibition.

Keywords

HERG MMPA Structure based design Synthesis Pharmacokinetics Covalent inhibitor Molecular complexity Cathepsin K

Related Topics

Physical Sciences and Engineering Chemistry Organic Chemistry

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Isosteric replacements for benzothiazoles and optimisation to potent Cathepsin K inhibitors free from hERG channel inhibition

Authors

Alexander G. Dossetter, Jonathan Bowyer, Calum R. Cook, James J. Crawford, Jonathan E. Finlayson, Nicola M. Heron, Christine Heyes, Adrian J. Highton, Julian A. Hudson, Anja Jestel, Stephan Krapp, Philip A. MacFaul, Thomas M. McGuire, Andrew D. Morley,