2017
DOI: 10.1016/j.bmc.2017.04.037
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A fragment-based approach leading to the discovery of a novel binding site and the selective CK2 inhibitor CAM4066

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Cited by 60 publications
(107 citation statements)
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“…Indeed, one such small pocket, termed αD pocket, was identified on the large C-terminal lobe of the catalytic subunit. 18 The most elaborated αD pocket ligand, CAM4712 (MW 453 g/mol), exhibited a moderate potency in the cell-free assay (IC 50 = 7 µM) and good efficacy in cells, while the selectivity over other kinases required further optimization. 19 modulators were investigated and compared to that of the ATP-competitive reference inhibitor CX-4945.…”
Section: Introductionmentioning
confidence: 99%
“…Indeed, one such small pocket, termed αD pocket, was identified on the large C-terminal lobe of the catalytic subunit. 18 The most elaborated αD pocket ligand, CAM4712 (MW 453 g/mol), exhibited a moderate potency in the cell-free assay (IC 50 = 7 µM) and good efficacy in cells, while the selectivity over other kinases required further optimization. 19 modulators were investigated and compared to that of the ATP-competitive reference inhibitor CX-4945.…”
Section: Introductionmentioning
confidence: 99%
“…CK2 α/β interface (Site 6 including Tyr 39, Val67, Val112 and Val101) has been confirmed to be occupied by the DRB, W16, CAM187 and cyclic peptide Pc, which antagonize the assembly of CK2 holoenzyme complex [16]. The αD pocket named site 3 was demonstrated as the allosteric pocket to accommodate the biaryl rings of CAM4712 analogues [17][18][19]. Recently, Bestgen et al discovered aminothiazole derivatives as the allosteric modulators of CK2 by targeting the interface between the αC helix and glycine-rich loop [20,21].…”
Section: Introductionmentioning
confidence: 90%
“…The structure-based pharmacophore model with 18 features was built based on the crystal structure of CK2α in complexed with compound 15 (compound number used in reference [19], PDB code: 5OTZ) using the "Interaction Generation" protocol in Discovery Studio 4.0. In order to optimize the pharmacophore model, ten active compounds reported in the literature were employed to hook the key pharmacophoric features as the positive set, and eight inactive compounds were used as the negative one [18,19] ( Figure S1a). Two hydrophobic features (HY22 and HY39) were recognized by all the ten active compounds, and two H-bond (hydrogen-bond) donor features (HBD32 and HBD96) were hooked by eight out of ten active compounds (Figure 2a).…”
Section: Structure-based Pharmacophore Modelingmentioning
confidence: 99%
“…Although often neglected, the impact on the ADMET properties should also be taken in consideration. In the case of the linker, that usually adds rotatable bonds to the system (Ichihara et al, 2011;De Fusco et al, 2017), this modification can lead to poor PK features, like low permeability (Veber et al, 2002).…”
Section: Linkingmentioning
confidence: 99%