過去の展示会情報をご覧いただけます。
- 2017年6月6日
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第17回日本蛋白質科学会年会(2017/6/20 – 22、仙台)
第17回日本蛋白質科学会年会(2017年6月20日~22日、仙台国際センター)に出展いたします。年会のページはこちら
第17回日本蛋白質科学会年会(2017/6/20 – 22、仙台)第17回日本蛋白質科学会年会(2017年6月20日~22日、仙台国際センター)に出展いたします。年会のページはこちら |
Database AutoPH4: pharmacophore analysis of multiple protein structures
Chris Williams (Chemical Computing Group ULC)
Abstract: An automated approach to summarize pocket shapes and binding hot-spots from a collection of protein structures is presented. Pocket shapes are described using pocket volumes derived from Alpha Sites and molecular surfaces. Binding hot-spots are located using pharmacophore features generated by AutoPH4. Collections of pocket volumes and pharmacophores are analyzed using feature densities which map onto a universal grid the fraction of structures that possess a given feature at each point in space. Regions with high pharmacophore feature densities identify the most persistent interaction binding hot-spots over the collection of structures. Pocket volume densities detect and classify binding site regions into core pockets and sub-pocket regions. Fingerprints that represent pocket shape, sub-pocket presence and pharmacophore feature presence are derived and used to cluster and classify multiple protein structures using standard fingerprint clustering tools. Application of the method to fragment-based drug design, minor pocket detection, selectivity mapping, binding-mode classification and custom docking scoring function creation is presented.