Crystal structure of human cyclin-dependent kinase-2 complex with MK2 inhibitor TEI-I01800: insight into the selectivity

Fujino, Aiko; Fukushima, Kei; Kubota, Takaharu; Kosugi, T.; Takimoto‐Kamimura, Midori

doi:10.1107/s0909049513020736

Cited by 6 publications

(5 citation statements)

References 27 publications

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“…These long hydrogen bonds could be the reason why TEI-L03090 shows weak inhibition. Furthermore, the interactions between Cys140 and TEI-I01800 are important for MK2 activity, as described in our previous study (Fujino et al, 2010(Fujino et al, , 2013Kosugi et al, 2012). TEI-L03090 lacked van der Waals contacts with Cys140 because TEI-L03090 lacks a substituent at the 8-position corresponding to the p-ethyoxyphenyl group at the 7-position of TEI-I01800.…”

Section: Resultsmentioning

confidence: 97%

“…TEI-I01800 is highly potent and selective against significant kinases and has a 177-fold selectivity for MK2 over CDK2 (its IC 50 values for MK2 and CDK2 are 0.13 and 23 mM, respectively). Furthermore, we have previously reported crystal structures of MK2 and CDK2 in complex with TEI-I01800 (Fujino et al, 2010(Fujino et al, , 2013Kosugi et al, 2012), which revealed that MK2-TEI-I01800 forms an uncommon -helical glycine-rich loop ( -form) which is induced by the stable conformer of TEI-I01800. On the other hand, CDK2-TEI-I01800 adopted the -form commonly observed in CDK2 complexes with a small inhibitor.…”

Section: Introductionmentioning

confidence: 99%

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Structure of the β-form of human MK2 in complex with the non-selective kinase inhibitor TEI-L03090

et al. 2013

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PDB reference: MK2-TEI-L03090 complex, 3wi6Mitogen-activated protein kinase-activated protein kinase 2 (MK2 or MAPKAP-K2), a serine/threonine kinase from the p38 mitogen-activated protein kinase signalling pathway, plays an important role in the production of TNF-and other cytokines. In a previous report, it was shown that MK2 in complex with the selective inhibitor TEI-I01800 adopts an -helical glycine-rich loop that is induced by the stable nonplanar conformer of TEI-I01800. To understand the mechanism of the structural change, the structure of MK2 bound to TEI-L03090, which lacks the key substituent found in TEI-I01800, was determined. MK2-TEI-L03090 has a -sheet glycine-rich loop in common with other kinases, as predicted. This result suggests that a small compound can induce a drastic conformational change in the target protein structure and can be used to design potent and selective inhibitors.

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Section: Resultsmentioning

confidence: 97%

Section: Introductionmentioning

confidence: 99%

Structure of the β-form of human MK2 in complex with the non-selective kinase inhibitor TEI-L03090

et al. 2013

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“…This unprofitable interaction pattern may be responsible for the lower affinity of 87 toward CDK2 in comparison to MK2 and consequently for its 177-fold kinase selectivity. 41 …”

Section: Crystallization Studiesmentioning

confidence: 99%

“…In the attempt to rationalize the kinase selectivity profile of 87 , analysis of its complex with CDK2 showed a strained conformation of the inhibitor that led to the lack of interactions between its substituent at the position 7 and the ATP binding site of CDK2, that assumed a β-sheet form. This unprofitable interaction pattern may be responsible for the lower affinity of 87 toward CDK2 in comparison to MK2 and consequently for its 177-fold kinase selectivity …”

Section: Crystallization Studiesmentioning

confidence: 99%

“…This unprofitable interaction pattern may be responsible for the lower affinity of 87 toward CDK2 in comparison to MK2 and consequently for its 177-fold kinase selectivity. 31 Another study demonstrated that, similarly to the complex between MK2 and 87, 28 2,4-diaminopyrimidine 80 induced the Gly-rich loop to assume an α-helical conformation (PDB entry 3ka0), 32 even if the Lys93-Glu104 salt bridge was maintained. On the contrary, the 2,4-diaminopyrimidine analogue 78 was cocrystallized with MK2 in the β-form (PDB entry 3kc3).…”

Section: Crystallization Studiesmentioning

confidence: 99%

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Targeting Mitogen-Activated Protein Kinase-Activated Protein Kinase 2 (MAPKAPK2, MK2): Medicinal Chemistry Efforts To Lead Small Molecule Inhibitors to Clinical Trials

2015

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The p38/MAPK-activated kinase 2 (MK2) pathway is involved in a series of pathological conditions (inflammation diseases and metastasis) and in the resistance mechanism to antitumor agents. None of the p38 inhibitors entered advanced clinical trials because of their unwanted systemic side effects. For this reason, MK2 was identified as an alternative target to block the pathway, but avoiding the side effects of p38 inhibition. However, ATP-competitive MK2 inhibitors suffered from low solubility, poor cell permeability, and scarce kinase selectivity. Fortunately, non-ATP-competitive inhibitors of MK2 have been already discovered that allowed circumventing the selectivity issue. These compounds showed the additional advantage to be effective at lower concentrations in comparison to the ATP-competitive inhibitors. Therefore, although the significant difficulties encountered during the development of these inhibitors, MK2 is still considered as an attractive target to treat inflammation and related diseases, to prevent tumor metastasis, and to increase tumor sensitivity to chemotherapeutics.

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Supercomputer docking with a large number of degrees of freedom

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et al. 2019

SAR and QSAR in Environmental Research

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Crystal structure of human cyclin-dependent kinase-2 complex with MK2 inhibitor TEI-I01800: insight into the selectivity

Cited by 6 publications

References 27 publications

Structure of the β-form of human MK2 in complex with the non-selective kinase inhibitor TEI-L03090

Structure of the β-form of human MK2 in complex with the non-selective kinase inhibitor TEI-L03090

Targeting Mitogen-Activated Protein Kinase-Activated Protein Kinase 2 (MAPKAPK2, MK2): Medicinal Chemistry Efforts To Lead Small Molecule Inhibitors to Clinical Trials

Supercomputer docking with a large number of degrees of freedom

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