Literature DB >> 25936518

The Ys and wherefores of protein kinase autoinhibition.

Richard Bayliss1, Tamanna Haq2, Sharon Yeoh2.   

Abstract

Protein phosphorylation is a key reaction in the regulation of cellular events and is catalysed by over 500 protein kinases in humans. The activities of protein kinases are strictly controlled through a diverse set of mechanisms. Structural studies have shown that the conformation adopted by kinases in their active state is highly similar, whereas inactive kinases can adopt a variety of conformations. Many kinases are maintained in a catalytically inactive state through autoinhibition. This involves a conformation of the kinase active site that is unable to support catalysis and requires activation through a signal such as binding of a regulatory protein. In this review, we briefly summarise some of the well-established autoinhibitory mechanisms and then focus on a relatively unexplored mode of autoinhibition that was first discovered in the Nek family of kinases and is also relevant to IRE1. This involves a tyrosine side-chain that blocks the active site and which must undergo a conformational change to enable kinase activity. We have termed this the Tyr-down autoinhibitory mechanism. We summarise the evidence for this mechanism and describe its role in kinase inhibitor design. Finally, we survey the kinome to identify other kinases with the potential to be governed by an autoinhibitory Tyr-down mechanism. This article is part of a Special Issue entitled: Inhibitors of Protein Kinases.
Copyright © 2015 Elsevier B.V. All rights reserved.

Entities:  

Keywords:  Phosphorylation; Regulation; Signaling; Structural biology

Mesh:

Substances:

Year:  2015        PMID: 25936518     DOI: 10.1016/j.bbapap.2015.04.025

Source DB:  PubMed          Journal:  Biochim Biophys Acta        ISSN: 0006-3002


  9 in total

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4.  Relief of autoinhibition by conformational switch explains enzyme activation by a catalytically dead paralog.

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6.  Binding to an Unusual Inactive Kinase Conformation by Highly Selective Inhibitors of Inositol-Requiring Enzyme 1α Kinase-Endoribonuclease.

Authors:  Giampiero Colombano; John J Caldwell; Thomas P Matthews; Chitra Bhatia; Amar Joshi; Tatiana McHardy; Ngai Yi Mok; Yvette Newbatt; Lisa Pickard; Jade Strover; Somaieh Hedayat; Michael I Walton; Stephanie M Myers; Alan M Jones; Harry Saville; Craig McAndrew; Rosemary Burke; Suzanne A Eccles; Faith E Davies; Richard Bayliss; Ian Collins
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7.  Mutation-oriented profiling of autoinhibitory kinase conformations predicts RAF inhibitor efficacies.

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8.  Conformational states dynamically populated by a kinase determine its function.

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9.  Nek7 conformational flexibility and inhibitor binding probed through protein engineering of the R-spine.

Authors:  Matthew J Byrne; Nazia Nasir; Christine Basmadjian; Chitra Bhatia; Rory F Cunnison; Katherine H Carr; Corine Mas-Droux; Sharon Yeoh; Céline Cano; Richard Bayliss
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  9 in total

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