AB668, a novel highly selective protein kinase CK2 inhibitor with a distinct anti-tumor mechanism as compared to CX-4945 and SGC-CK2-1

Author:

Bancet AlexandreORCID,Frem RitaORCID,Jeanneret FlorianORCID,Mularoni AngéliqueORCID,Bazelle Pauline,Roelants CarolineORCID,Delcros Jean-GuyORCID,Guichou Jean-FrançoisORCID,Pillet Catherine,Coste IsabelleORCID,Renno TouficORCID,Battail ChristopheORCID,Cochet ClaudeORCID,Lomberget ThierryORCID,Filhol OdileORCID,Krimm IsabelleORCID

Abstract

AbstractAlthough the involvement of protein kinase CK2 in cancer is well-documented, there is a need for selective CK2 inhibitors suitable for investigating CK2 specific roles in cancer-related biological pathways and further explore its therapeutic potential. Here we have discovered AB668, a new bivalent inhibitor that binds both at the ATP site and an allosteric αD pocket unique to CK2. The molecule inhibits CK2 activity with an outstanding selectivity over other kinases. Using caspase activation assay, live-cell imaging and transcriptomic analysis, we have compared the effects of this bivalent inhibitor to the non-selective ATP-competitive inhibitor CX-4945 that reached clinic and to the selective ATP-competitive SGC-CK2-1 molecule. Our results show that in contrast to CX-4945 or SGC-CK2-1, AB668 has a distinct mechanism of action regarding its anti-cancer activity, inducing apoptotic cell death and stimulating distinct biological pathways in several cancer cell lines while sparing healthy cells. Our data suggest that targeting a cryptic CK2 αD pocket validates an allosteric approach to targeting CK2 and provides a starting point for creating drug-like CK2 inhibitors for aggressive cancers.

Publisher

Cold Spring Harbor Laboratory

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