| Literature DB >> 28075591 |
Victoria A Steadman1, Simon B Pettit1, Karine G Poullennec1, Linos Lazarides1, Andrew J Keats1, David K Dean1, Steven J Stanway1, Carol A Austin1, Jonathan A Sanvoisin1, Gregory M Watt1, Hans G Fliri2, Albert C Liclican3, Debi Jin3, Melanie H Wong3, Stephanie A Leavitt3, Yu-Jen Lee3, Yang Tian3, Christian R Frey3, Todd C Appleby3, Uli Schmitz3, Petr Jansa3, Richard L Mackman3, Brian E Schultz3.
Abstract
Cyclophilin inhibition has been a target for the treatment of hepatitis C and other diseases, but the generation of potent, drug-like molecules through chemical synthesis has been challenging. In this study, a set of macrocyclic cyclophilin inhibitors was synthesized based on the core structure of the natural product sanglifehrin A. Initial compound optimization identified the valine-m-tyrosine-piperazic acid tripeptide (Val-m-Tyr-Pip) in the sanglifehrin core, stereocenters at C14 and C15, and the hydroxyl group of the m-tyrosine (m-Tyr) residue as key contributors to compound potency. Replacing the C18-C21 diene unit of sanglifehrin with a styryl group led to potent compounds that displayed a novel binding mode in which the styrene moiety engaged in a π-stacking interaction with Arg55 of cyclophilin A (Cyp A), and the m-Tyr residue was displaced into solvent. This observation allowed further simplifications of the scaffold to generate new lead compounds in the search for orally bioavailable cyclophilin inhibitors.Entities:
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Year: 2017 PMID: 28075591 DOI: 10.1021/acs.jmedchem.6b01329
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446