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  4. Structures of P. falciparum PfPK5 test the CDK regulation paradigm and suggest mechanisms of small molecule inhibition
 
research article

Structures of P. falciparum PfPK5 test the CDK regulation paradigm and suggest mechanisms of small molecule inhibition

Holton, Simon
•
Merckx, Anais
•
Burgess, Darren
Show more
2003
Structure

Plasmodium falciparum cell cycle regulators are promising targets for antimalarial drug design. We have determined the structure of PfPK5, the first structure of a P. falciparum protein kinase and the first of a cyclin-dependent kinase (CDK) not derived from humans. The fold and the mechanism of inactivation of monomeric CDKs are highly conserved across evolution. ATP-competitive CDK inhibitors have been developed as potential leads for cancer therapeutics. These studies have identified regions of the CDK active site that can be exploited to achieve significant gains in inhibitor potency and selectivity. We have cocrystallized PfPK5 with three inhibitors that target such regions. The sequence differences between PfPK5 and human CDKs within these inhibitor binding sites suggest that selective inhibition is an attainable goal. Such compounds will be useful tools for P. falciparum cell cycle studies, and will provide lead compounds for antimalarial drug development.

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Type
research article
DOI
10.1016/j.str.2003.09.020
Author(s)
Holton, Simon
Merckx, Anais
Burgess, Darren
Doerig, Christian  
Noble, Martin
Endicott, Jane
Date Issued

2003

Published in
Structure
Volume

11

Issue

11

Start page

1329

End page

37

Subjects

Gene Expression Regulation, Enzymologic

Editorial or Peer reviewed

REVIEWED

Written at

OTHER

EPFL units
INSERM-EPFL  
Available on Infoscience
April 14, 2010
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/49379
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