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Serendipitous discovery of novel bacterial methionine aminopeptidase inhibitors |
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| Authors: | Evdokimov Artem G Pokross Matthew Walter Richard L Mekel Marlene Barnett Bobby L Amburgey Jack Seibel William L Soper Shari J Djung Jane F Fairweather Neil Diven Conrad Rastogi Vinit Grinius Leo Klanke Charles Siehnel Richard Twinem Tracy Andrews Ryan Curnow Alan |
| Institution: | Structural Biology Core Facility, The Procter & Gamble Pharmaceuticals, Mason, Ohio 45040, USA. artem@xtals.org |
| Abstract: | In this article we describe the application of structural biology methods to the discovery of novel potent inhibitors of methionine aminopeptidases. These enzymes are employed by the cells to cleave the N-terminal methionine from nascent peptides and proteins. As this is one of the critical steps in protein maturation, it is very likely that inhibitors of these enzymes may prove useful as novel antibacterial agents. Involvement of crystallography at the very early stages of the inhibitor design process resulted in serendipitous discovery of a new inhibitor class, the pyrazole-diamines. Atomic-resolution structures of several inhibitors bound to the enzyme illuminate a new mode of inhibitor binding. |
| Keywords: | structure‐based drug design virtual screening antibacterial methionine aminopeptidase |
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