Review
Nature Reviews Drug Discovery 3, 660-672 (August 2004) | doi:10.1038/nrd1467
Fragment-based lead discovery
David C. Rees1, Miles Congreve,1, Christopher W. Murray1 & Robin Carr1 About the authors
Abstract
Fragment-based lead discovery is gaining momentum in both large pharmaceutical companies and biotechnology laboratories as a complementary approach to traditional screening. This is because fragment-based approaches require significantly fewer compounds to be screened and synthesized, and are showing a high success rate in generating chemical series with lead-like properties. Compared with traditional screening hits, the starting fragments have considerably lower molecular mass, and although the binding interactions of these fragments with a target protein are weak, they are structurally understood through X-ray crystallography or NMR, and they exhibit high 'ligand efficiency'. Here, we use examples from 25 different protein targets to describe chemical strategies that exploit this structural knowledge to rapidly develop fragments into high-affinity leads.
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Author affiliations
- Astex Technology, 436 Cambridge Science Park, Milton Road, Cambridge CB4 0QA, UK.
Correspondence to: David C. Rees1 Email: d.rees@astex-technology.com
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