Current perspectives in fragment-based lead discovery (FBLD)

Author:

Lamoree Bas1,Hubbard Roderick E.12

Affiliation:

1. York Structural Biology Laboratory (YSBL), Department of Chemistry, University of York, Heslington, York YO10 5DD, U.K.

2. Vernalis Research, Granta Park, Abington, Cambridge CB21 6GB, U.K.

Abstract

It is over 20 years since the first fragment-based discovery projects were disclosed. The methods are now mature for most ‘conventional’ targets in drug discovery such as enzymes (kinases and proteases) but there has also been growing success on more challenging targets, such as disruption of protein–protein interactions. The main application is to identify tractable chemical startpoints that non-covalently modulate the activity of a biological molecule. In this essay, we overview current practice in the methods and discuss how they have had an impact in lead discovery – generating a large number of fragment-derived compounds that are in clinical trials and two medicines treating patients. In addition, we discuss some of the more recent applications of the methods in chemical biology – providing chemical tools to investigate biological molecules, mechanisms and systems.

Publisher

Portland Press Ltd.

Subject

Molecular Biology,Biochemistry

Reference56 articles.

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