Identification of polyoxometalates as nanomolar noncompetitive inhibitors of protein kinase CK2 |
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| Authors: | Prudent Renaud Moucadel Virginie Laudet Béatrice Barette Caroline Lafanechère Laurence Hasenknopf Bernold Li Joaquim Bareyt Sébastian Lacôte Emmanuel Thorimbert Serge Malacria Max Gouzerh Pierre Cochet Claude |
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| Affiliation: | Laboratoire de Transduction du Signal, Institut de Recherche en Technologies et Sciences pour le Vivant, CEA, 17 Rue des Martyrs 38054 Grenoble, France. |
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| Abstract: | Protein kinase CK2 is a multifunctional kinase of medical importance that is dysregulated in many cancers. In this study, polyoxometalates were identified as original CK2 inhibitors. [P2Mo18O62](6-) has the most potent activity. It inhibits the kinase in the nanomolar range by targeting key structural elements located outside the ATP- and peptide substrate-binding sites. Several polyoxometalate derivatives exhibit strong inhibitory efficiency, with IC50 values < or = 10 nM. Furthermore, these inorganic compounds show a striking specificity for CK2 when tested in a panel of 29 kinases. Therefore, polyoxometalates are effective CK2 inhibitors in terms of both efficiency and selectivity and represent nonclassical kinase inhibitors that interact with CK2 in a unique way. This binding mode may provide an exploitable mechanism for developing potent drugs with desirable properties, such as enhanced selectivity relative to ATP-mimetic inhibitors. |
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| Keywords: | CHEMBIO SIGNALING |
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