Open AccessFree Ligand 1D NMR Conformational Signatures To Enhance Structure Based Drug Design of a Mcl-1 Inhibitor (AZD5991) and Other Synthetic Macrocycles
Author(s) -
Amber Balazs,
Rodrigo J. Carbajo,
Nichola L. Davies,
Yu Dong,
Alexander W. Hird,
Jeffrey W. Johannes,
Michelle L. Lamb,
William McCoull,
Piotr Raubo,
Graeme R. Robb,
Martin J. Packer,
Elisabetta Chiarparin
Publication year - 2019
Publication title -
journal of medicinal chemistry
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 2.01
H-Index - 261
eISSN - 1520-4804
pISSN - 0022-2623
DOI - 10.1021/acs.jmedchem.9b00716
Subject(s) - chemistry , ligand (biochemistry) , combinatorial chemistry , stereochemistry , nuclear magnetic resonance spectroscopy , drug discovery , two dimensional nuclear magnetic resonance spectroscopy , biochemistry , receptor
The three-dimensional conformations adopted by a free ligand in solution impact bioactivity and physicochemical properties. Solution 1D NMR spectra inherently contain information on ligand conformational flexibility and three-dimensional shape, as well as the propensity of the free ligand to fully preorganize into the bioactive conformation. Herein we discuss some key learnings, distilled from our experience developing potent and selective synthetic macrocyclic inhibitors, including Mcl-1 clinical candidate AZD5991. Case studies have been selected from recent oncology research projects, demonstrating how 1D NMR conformational signatures can complement X-ray protein-ligand structural information to guide medicinal chemistry optimization. Learning to extract free ligand conformational information from routinely available 1D NMR signatures has proven to be fast enough to guide medicinal chemistry decisions within design cycles for compound optimization.
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