2023
DOI: 10.1016/j.isci.2022.105806
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Temporal phosphoproteomics reveals WEE1-dependent control of 53BP1 pathway

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Cited by 8 publications
(7 citation statements)
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“…To evaluate the potential synergistic effect of co-targeting WEE1 and PKMYT1, we conducted a dose response matrix for cell viability with the WEE1 inhibitor adavosertib in combination with the PKMYT1 inhibitor RP-6306 (Figure 1A and B ). The U2OS cell line was selected as a model since it has been well characterized for WEE1 and CDK functions, and notably, investigated in detail for the effects of adavosertib treatment ( 33 ). At 100 nM concentration, the combinatorial treatment led to efficient killing of most U2OS cells (Figure 1B ).…”
Section: Resultsmentioning
confidence: 99%
“…To evaluate the potential synergistic effect of co-targeting WEE1 and PKMYT1, we conducted a dose response matrix for cell viability with the WEE1 inhibitor adavosertib in combination with the PKMYT1 inhibitor RP-6306 (Figure 1A and B ). The U2OS cell line was selected as a model since it has been well characterized for WEE1 and CDK functions, and notably, investigated in detail for the effects of adavosertib treatment ( 33 ). At 100 nM concentration, the combinatorial treatment led to efficient killing of most U2OS cells (Figure 1B ).…”
Section: Resultsmentioning
confidence: 99%
“…Similar results were obtained when WEE1 was depleted using siRNA, confirming that WEE1 kinase is the main target of AZD1775 (Figure 2-figure supplement 1H). We then investigated the impact of CDK1 and CDK2, the major kinases controlled by WEE1 31 . The abnormal mitosis phenotype was completely abolished upon combining WEE1 inhibition with RO-3306, a CDK1 inhibitor (Figure 2-figure supplement 1I,J) but not following CDK2 depletion (Figure 2-figure supplement 1K), confirming that the abnormal phenotype was mainly due to the activation of CDK1 after WEE1 inhibition.…”
Section: Resultsmentioning
confidence: 99%
“…WEE1 supports genome integrity by suppressing excessive origin firing during DNA replication and premature entry into mitosis [5][6][7]. Consequently, inhibition of WEE1 removes the negative phosphorylation on CDK1/2 (in concert with CDC25) resulting in deregulation of CDKs, increased origin firing and replication fork degradation leading to fork collapse, DNA damage, and unscheduled mitosis [1,[8][9][10]. Recent studies show that WEE1 inhibition by AZD1775 (Adavosertib), a potent and specific small-molecule inhibitor, alone or in combination with DNA damaging agents effectively kills cancer cells of various origins [8,11,12].…”
Section: Introductionmentioning
confidence: 99%