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. 2017 Sep 26;15(37):7729-7735.
doi: 10.1039/c7ob00056a.

Progress towards the broad use of non-peptide synthetic macrocycles in drug discovery

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Progress towards the broad use of non-peptide synthetic macrocycles in drug discovery

Adrian Whitty et al. Org Biomol Chem. .

Abstract

We discuss progress towards addressing three key questions pertaining to the design of screening libraries of synthetic non-peptidic macrocycles (MCs) for drug discovery: What structural and physicochemical properties of MCs maximize the likelihood of achieving strong and specific binding to protein targets? What features render a protein target suitable for binding MCs, and can this information be used to identify suitable targets for inhibition by MCs? What properties of synthetic MCs confer good pharmaceutical properties, and particularly good aqueous solubility coupled with passive membrane permeability? We additionally discuss how the criteria that define a meaningful MC screening hit are linked to the size of the screening library and the synthetic methodology employed in its preparation.

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