Accelerating Drug Discovery With High‐Throughput Crystallographic Fragment Screening and Structural Enablement

Fragment‐based drug discovery is a well‐established method for the identification of chemical starting points for development into clinical candidates. Historically, crystallographic fragment screening was perceived to be low‐throughput and time consuming. However, thanks to advances in synchrotron...

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Veröffentlicht in:	Applied Research 2024-11
Hauptverfasser:	Fearon, Daren, Powell, Ailsa, Douangamath, Alice, Dias, Alexandre, Tomlinson, Charles W. E., Balcomb, Blake H., Aschenbrenner, Jasmin C., Aimon, Anthony, Barker, Isabel A., Brandão‐Neto, José, Collins, Patrick, Dunnett, Louise E., Fairhead, Michael, Gildea, Richard J., Golding, Mathew, Gorrie‐Stone, Tyler, Hathaway, Paul V., Koekemoer, Lizbé, Krojer, Tobias, Lithgo, Ryan M., Maclean, Elizabeth M., Marples, Peter G., Ni, Xiaomin, Skyner, Rachael, Talon, Romain, Thompson, Warren, Wild, Conor F., Winokan, Max, Wright, Nathan David, Winter, Graeme, Shotton, Elizabeth J., von Delft, Frank
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creator	Fearon, Daren Powell, Ailsa Douangamath, Alice Dias, Alexandre Tomlinson, Charles W. E. Balcomb, Blake H. Aschenbrenner, Jasmin C. Aimon, Anthony Barker, Isabel A. Brandão‐Neto, José Collins, Patrick Dunnett, Louise E. Fairhead, Michael Gildea, Richard J. Golding, Mathew Gorrie‐Stone, Tyler Hathaway, Paul V. Koekemoer, Lizbé Krojer, Tobias Lithgo, Ryan M. Maclean, Elizabeth M. Marples, Peter G. Ni, Xiaomin Skyner, Rachael Talon, Romain Thompson, Warren Wild, Conor F. Winokan, Max Wright, Nathan David Winter, Graeme Shotton, Elizabeth J. von Delft, Frank
description	Fragment‐based drug discovery is a well‐established method for the identification of chemical starting points for development into clinical candidates. Historically, crystallographic fragment screening was perceived to be low‐throughput and time consuming. However, thanks to advances in synchrotron capabilities and the introduction of dedicated facilities, such as the XChem platform at Diamond Light Source, there have been substantial improvements in throughput and integration between sample preparation, data collection and hit identification. Herein we share our experiences of establishing a crystallographic fragment screening facility, our learnings from operating a user programme for ten years and our perspective on applying structural enablement to rapidly progress initial fragment hits to lead‐like molecules.
doi_str_mv	10.1002/appl.202400192
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title	Accelerating Drug Discovery With High‐Throughput Crystallographic Fragment Screening and Structural Enablement
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