Fragment Screening of Infectious Disease Targets in a Structural Genomics Environment

Structural genomics efforts have traditionally focused on generating single protein structures of unique and diverse targets. However, a lone structure for a given target is often insufficient to firmly assign function or to drive drug discovery. As part of the Seattle Structural Genomics Center for...

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Veröffentlicht in:Methods in Enzymology 2011-01, Vol.493, p.533-556
Hauptverfasser: Begley, Darren W., Davies, Douglas R., C. Hartley, Robert, Edwards, Thomas E., Staker, Bart L., Van Voorhis, Wesley C., Myler, Peter J., Stewart, Lance J.
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Sprache:eng
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Zusammenfassung:Structural genomics efforts have traditionally focused on generating single protein structures of unique and diverse targets. However, a lone structure for a given target is often insufficient to firmly assign function or to drive drug discovery. As part of the Seattle Structural Genomics Center for Infectious Disease (SSGCID), we seek to expand the focus of structural genomics by elucidating ensembles of structures that examine small molecule–protein interactions for selected infectious disease targets. In this chapter, we discuss two applications for small molecule libraries in structural genomics: unbiased fragment screening, to provide inspiration for lead development, and targeted, knowledge-based screening, to confirm or correct the functional annotation of a given gene product. This shift in emphasis results in a structural genomics effort that is more engaged with the infectious disease research community, and one that produces structures of greater utility to researchers interested in both protein function and inhibitor development. We also describe specific methods for conducting high-throughput fragment screening in a structural genomics context by X-ray crystallography.
ISSN:0076-6879
1557-7988
DOI:10.1016/B978-0-12-381274-2.00021-2