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. 2014 Jul 21;53(30):7828-31.
doi: 10.1002/anie.201404301. Epub 2014 Jun 5.

Macrocyclic protease inhibitors with reduced peptide character

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Macrocyclic protease inhibitors with reduced peptide character

Krystle C H Chua et al. Angew Chem Int Ed Engl. .

Abstract

There is a real need for simple structures that define a β-strand conformation, a secondary structure that is central to peptide-protein interactions. For example, protease substrates and inhibitors almost universally adopt this geometry on active site binding. A planar pyrrole is used to replace two amino acids of a peptide backbone to generate a simple macrocycle that retains the required geometry for active site binding. The resulting β-strand templates have reduced peptide character and provide potent protease inhibitors with the attachment of an appropriate amino aldehyde to the C-terminus. Picomolar inhibitors of cathepsin L and S are reported and the mode of binding of one example to the model protease chymotrypsin is defined by X-ray crystallography.

Keywords: inhibitors; macrocycles; peptidomimetics; proteases; β-strands.

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