Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: EC:2.7.11.22 (
cdc2
)
8,319
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Selective protein kinase inhibitors were developed on the basis of the unexpected binding mode of 2,6,9-trisubstituted purines to the adenosine triphosphate-binding site of the human cyclin-dependent kinase 2 (CDK2). By iterating chemical library synthesis and biological screening, potent inhibitors of the human CDK2-cyclin A kinase complex and of Saccharomyces cerevisiae
Cdc28p
were identified. The structural basis for the binding affinity and selectivity was determined by analysis of a three-dimensional crystal structure of a CDK2-inhibitor complex. The cellular effects of these compounds were characterized in mammalian cells and yeast. In the latter case the effects were characterized on a genome-wide scale by monitoring changes in messenger RNA levels in treated cells with high-density oligonucleotide probe arrays.
Purine
libraries could provide useful tools for analyzing a variety of signaling and regulatory pathways and may lead to the development of new therapeutics.
...
PMID:Exploiting chemical libraries, structure, and genomics in the search for kinase inhibitors. 967 90
The cell division cycle is controlled by cyclin-dependent kinases (cdk), which consist of a catalytic subunit (
cdk1
-
cdk8
) and a regulatory subunit (cyclin A-H).
Purine
-like inhibitors of cyclin-dependent kinases have recently been found to be of potential use as anticancer drugs. Rigid and flexible docking techniques were used for analysis of binding mode and design of new inhibitors. X-ray structures of three (ATP, olomoucine, roscovitine)
cdk2
complexes were available at the beginning of the study and were used to optimize the docking parameters. The new potential inhibitors were then docked into the
cdk2
enzyme, and the enzyme/inhibitor interaction energies were calculated and tested against the assayed activities of
cdk1
(37 compounds) and
cdk2
(9 compounds). A significant rank correlation between the activity and the rigid docking interaction energy has been found. This implies that (i) the rigid docking can be used as a tool for qualitative prediction of activity and (ii) values obtained by the rigid docking technique into the
cdk2
active site can also be used for the prediction of
cdk1
activity. While the resulting geometries obtained by the rigid docking are in good agreement with the X-ray data, the flexible docking did not always produce the same inhibitor conformation as that found in the crystal.
...
PMID:Docking-based development of purine-like inhibitors of cyclin-dependent kinase-2. 1089 Nov 9
Purine
inhibitors of cyclin-dependent kinases attract attention as potential anticancer drugs because their first representative roscovitine recently entered clinical trials. Although well described in terms of structure-activity relationships, we still present here a novel modification of the purine scaffold influencing their inhibitory properties. The introduced C-8 substituents, however, lowered the
CDK
inhibitory activity of roscovitine, whereas the antiproliferative potential of several derivatives remained high.
...
PMID:2,6,8,9-tetrasubstituted purines as new CDK1 inhibitors. 1294 19
