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1 Chk1 kinase inhibitors are currently under clinical inve
2 lay only briefly in CPT medium by activating Chk1 kinase, cdc2.1w cells bypass Chk1 to enter an exten
5 inding interactions between compound 46b and Chk1 kinase, revealed by X-ray cocrystal structure, were
6 gamma-H2AX, replication protein A foci, and Chk1 kinase phosphorylation, a readout for activation of
7 examined the respective roles of the ATR and Chk1 kinases in ovarian cancer cells using genetic and p
8 n abrogates IR-induced activation of ATR and Chk1 kinases, as well as phosphorylation of Cdc2-Tyr15,
11 giectecia-mutated and Rad3-related (ATR) and Chk1 kinases and inhibition of Cdc2/Cyclin B activity.
12 elements in the signaling network (Myt1 and Chk1 kinases), and fits a large and diverse body of data
14 t activation involves activation of Wee1 and Chk1 kinases and inhibition of Cdc25A and Cdc25C phospha
18 transmit DNA damage signals through the ATR-Chk1 kinase cascade, whether post-translational modifica
20 egulation in BER-depleted cells requires ATR/Chk1 kinase activities, demonstrating that PD-L1 upregul
23 SUMOylation occurs in cells with compromised Chk1 kinase activity, necessary for known posttranslatio
25 system in which the phosphorylation of human Chk1 kinase by ATR (ataxia telangiectasia mutated and Ra
26 A resolution crystal structures of the human Chk1 kinase domain and its binary complex with an ATP an
31 ive indolocarbazole inhibitor (SB-218078) of Chk1 kinase activity and used this compound to assess ce
33 is suggests the expression and activation of Chk1 kinase is associated with cells undergoing active D
39 excision repair leads to phosphorylation of Chk1 kinase in both G1 and S phase of the cell cycle, su
41 s a homolog of the Schizosaccharomyces pombe Chk1 kinase, provides a cell-cycle checkpoint that delay
47 w that BRCA1 is essential for activating the Chk1 kinase that regulates DNA damage-induced G2/M arres
48 o demonstrate that serine 83 of Mcd1 and the Chk1 kinase are critical determinants for DSB-induced co
52 role of Cdc2 tyrosine phosphorylation in the Chk1 kinase-mediated DNA damage checkpoint has remained
55 cation checkpoint and phosphorylation of the Chk1 kinase are dependent on RNA primer synthesis by DNA
56 tion specifically destroys regulation of the Chk1 kinase but not the Chk2 kinase, suggesting involvem