Enzyme Tunnels and Gates As Relevant Targets in Drug Design

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Authors

MARQUES Sérgio Manuel DANIEL Lukáš BURYŠKA Tomáš PROKOP Zbyněk BREZOVSKÝ Jan DAMBORSKÝ Jiří

Year of publication 2017
Type Article in Periodical
Magazine / Source MEDICINAL RESEARCH REVIEWS
MU Faculty or unit

Faculty of Science

Citation
Web https://loschmidt.chemi.muni.cz/peg/wp-content/uploads/2016/12/Marques_16res_rev.pdf
Doi http://dx.doi.org/10.1002/med.21430
Keywords drug design; protein tunnels; protein gates; drug binding; selectivity; specificity
Description Many enzymes contain tunnels and gates that are essential to their function. Gates reversibly switch between open and closed conformations and thereby control the traffic of small molecules-substrates, products, ions, and solvent molecules-into and out of the enzyme's structure via molecular tunnels. Many transient tunnels and gates undoubtedly remain to be identified, and their functional roles and utility as potential drug targets have received comparatively little attention. Here, we describe a set of general concepts relating to the structural properties, function, and classification of these interesting structural features. In addition, we highlight the potential of enzyme tunnels and gates as targets for the binding of small molecules. The different types of binding that are possible and the potential pharmacological benefits of such targeting are discussed. Twelve examples of ligands bound to the tunnels and/or gates of clinically relevant enzymes are used to illustrate the different binding modes and to explain some new strategies for drug design. Such strategies could potentially help to overcome some of the problems facing medicinal chemists and lead to the discovery of more effective drugs.
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