2017
DOI: 10.1002/cmdc.201600535
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Inhibitor Selectivity for Cyclin‐Dependent Kinase 7: A Structural, Thermodynamic, and Modelling Study

Abstract: Table of contents entryWe have solved crystal structures of CDK7--selective inhibitors bound to CDK2.We have used a combination of structural, biophysical and modelling approaches to model the binding of these inhibitors to CDK7, and have used this information to explain their selectivity. We identify specific CDK7 residues that contribute to these inhibitors' specificity. AbstractDeregulation of the cell cycle by mechanisms that lead to elevated activities of cyclin--dependent kinases (CDK) is a feature of ma… Show more

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Cited by 34 publications
(35 citation statements)
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References 48 publications
(126 reference statements)
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“…Recently, in silico modeling of BS-181 and related compounds with the crystal structure of CDK7 led to the development of ICEC0942, an analog of BS-181 with improved cell permeability and oral bioavailability [50,51]. ICEC0942 inhibited growth of all NCI-60 cancer cell lines, with a median GI 50 of 0.25 µM [51].…”
Section: Bs-181 and Icec0942mentioning
confidence: 99%
“…Recently, in silico modeling of BS-181 and related compounds with the crystal structure of CDK7 led to the development of ICEC0942, an analog of BS-181 with improved cell permeability and oral bioavailability [50,51]. ICEC0942 inhibited growth of all NCI-60 cancer cell lines, with a median GI 50 of 0.25 µM [51].…”
Section: Bs-181 and Icec0942mentioning
confidence: 99%
“…OMEGA was used to generate up to 200 conformers per compound and provides the multi‐conformer database required for FRED docking. Using the Pdb2Receptor tool, a CDK2 binding pocket was prepared from a co‐crystal structure (PDBID 5JQ5) and the designed molecules were docked to the CDK2 binding pocket. The docking condition was determined by following procedure.…”
Section: Methodsmentioning
confidence: 99%
“…A number of selective small molecule inhibitors of CDK7 have been developed. These include the pyrazolopyrimidine derivatives, BS-181 [39] and ICEC0942 [22,107], and the pyrazolotriazine derivatives, LDC4297 [108] and QS1189 [109] (Fig. 3b, Table 3).…”
Section: Cdk7-specific Inhibitorsmentioning
confidence: 99%
“…Efforts to develop BS-181 analogues which retain CDK7 selectivity, but have improved drug-like properties, led to the first orally bioavailable CDK7 inhibitor, ICEC0942 (CT7001; Fig. 3b, Table 3) [22,107]. Although crystal structures of CDK7 bound to ICEC0942 could not be obtained, a crystal structure of CDK2 in complex with ICEC0942 was solved [107].…”
Section: Cdk7-specific Inhibitorsmentioning
confidence: 99%