| Literature DB >> 28234462 |
Yuezhou Zhang, Alexandre Borrel1, Leo Ghemtio, Leslie Regad1, Gustav Boije Af Gennäs, Anne-Claude Camproux1, Jari Yli-Kauhaluoma, Henri Xhaard.
Abstract
We developed a computational workflow to mine the Protein Data Bank for isosteric replacements that exist in different binding site environments but have not necessarily been identified and exploited in compound design. Taking phosphate groups as examples, the workflow was used to construct 157 data sets, each composed of a reference protein complexed with AMP, ADP, ATP, or pyrophosphate as well other ligands. Phosphate binding sites appear to have a high hydration content and large size, resulting in U-shaped bioactive conformations recurrently found across unrelated protein families. A total of 16 413 replacements were extracted, filtered for a significant structural overlap on phosphate groups, and sorted according to their SMILES codes. In addition to the classical isosteres of phosphate, such as carboxylate, sulfone, or sulfonamide, unexpected replacements that do not conserve charge or polarity, such as aryl, aliphatic, or positively charged groups, were found.Entities:
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Year: 2017 PMID: 28234462 DOI: 10.1021/acs.jcim.6b00519
Source DB: PubMed Journal: J Chem Inf Model ISSN: 1549-9596 Impact factor: 4.956