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• W2011897955 abstract "Drug design methods have made significant new advances over the last ten years, mainly in the areas of molecular modelling. In more recent times important developments in theory have led to a different type of modelling becoming possible, the so-called de novo or automated design algorithms. In this new method the programs perform much of the chemist's thinking, in finding appropriately sized chemical groups to fit into a target site. However this is a combinatoric problem which has no general analytical solution; it is ripe for optimization. Other advances, such as combinatorial chemical synthesis and screening, will dramatically influence the search for new lead structures for target sites, which at present are poorly understood. Already these methods are being applied to peptide libraries. Peptides do not make good drug compounds because of their poor bioavailability; further, their flexibility reduces their affinity. In some cases peptide backbones can be removed and replaced with rigid non-peptide scaffolds." @default.
• W2011897955 created "2016-06-24" @default.
• W2011897955 creator A5044619755 @default.
• W2011897955 date "1994-09-01" @default.
• W2011897955 modified "2023-09-23" @default.
• W2011897955 title "Recent advances in drug design methods: Where will they lead?" @default.
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• W2011897955 doi "https://doi.org/10.1002/bies.950160915" @default.
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