A unified lead-oriented synthesis of over fifty molecular scaffolds

Richard G. Doveston; Paolo Tosatti; Mark Dow; Daniel J. Foley; Ho Yin Li; Amanda J. Campbell; David House; Ian Churcher; Stephen P. Marsden; Adam Nelson

doi:10.1039/C4OB02287D

A unified lead-oriented synthesis of over fifty molecular scaffolds†

Richard G. Doveston,^a Paolo Tosatti,^a Mark Dow,^a Daniel J. Foley,^a Ho Yin Li,^a Amanda J. Campbell,^b David House,^b Ian Churcher,^b Stephen P. Marsden*^a and Adam Nelson*^ac

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^a School of Chemistry, University of Leeds, Leeds, UK
E-mail: s.p.marsden@leeds.ac.uk, a.s.nelson@leeds.ac.uk

^b GlaxoSmithKline Medicines Research Centre, Stevenage, UK

^c Astbury Centre for Structural Molecular Biology, University of Leeds, Leeds, UK

Abstract

Controlling the properties of lead molecules is critical in drug discovery, but sourcing large numbers of lead-like compounds for screening collections is a major challenge. A unified synthetic approach is described that enabled the synthesis of 52 diverse lead-like molecular scaffolds from a minimal set of 13 precursors. The divergent approach exploited a suite of robust, functional group-tolerant transformations. Crucially, after derivatisation, these scaffolds would target significant lead-like chemical space, and complement commercially-available compounds.

Organic & Biomolecular Chemistry

A unified lead-oriented synthesis of over fifty molecular scaffolds†

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A unified lead-oriented synthesis of over fifty molecular scaffolds

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