Unknown

Dataset Information

0

Inhibition of Wee1 sensitizes cancer cells to antimetabolite chemotherapeutics in vitro and in vivo, independent of p53 functionality.

ABSTRACT: Inhibition of Wee1 is emerging as a novel therapeutic strategy for cancer, and some data suggest that cells with dysfunctional p53 are more sensitive to Wee1 inhibition combined with conventional chemotherapy than those with functional p53. We and others found that Wee1 inhibition sensitizes leukemia cells to cytarabine. Thus, we sought to determine whether chemosensitization by Wee1 inhibition is dependent on p53 dysfunction and whether combining Wee1 inhibition is tolerable and effective in vivo. Synergistic inhibition of proliferation with a Wee1 inhibitor in clinical development, MK1775, and cytarabine was observed in all acute myelogenous leukemia (AML) cell lines tested, regardless of p53 functionality. Mechanistic studies indicate that inhibition of Wee1 abrogates the S-phase checkpoint and augments apoptosis induced by cytarabine. In AML and lung cancer cell lines, genetic disruption of p53 did not alter the cells' enhanced sensitivity to antimetabolites with Wee1 inhibition. Finally, mice with AML were treated with cytarabine and/or MK1775. The combination of MK1775 and cytarabine was well tolerated in mice and enhanced the antileukemia effects of cytarabine, including survival. Thus, inhibition of Wee1 sensitizes hematologic and solid tumor cell lines to antimetabolite chemotherapeutics, whether p53 is functional or not, suggesting that the use of p53 mutation as a predictive biomarker for response to Wee1 inhibition may be restricted to certain cancers and/or chemotherapeutics. These data provide preclinical justification for testing MK1775 and cytarabine in patients with leukemia.

SUBMITTER: Van Linden AA 

PROVIDER: S-EPMC3897395 | biostudies-literature | 2013 Dec

REPOSITORIES: biostudies-literature

Json Xml
altmetric image

Publications

Inhibition of Wee1 sensitizes cancer cells to antimetabolite chemotherapeutics in vitro and in vivo, independent of p53 functionality.

Van Linden Annemie A AA   Baturin Dmitry D   Ford James B JB   Fosmire Susan P SP   Gardner Lori L   Korch Christopher C   Reigan Philip P   Porter Christopher C CC  

Molecular cancer therapeutics 20131011 12

Inhibition of Wee1 is emerging as a novel therapeutic strategy for cancer, and some data suggest that cells with dysfunctional p53 are more sensitive to Wee1 inhibition combined with conventional chemotherapy than those with functional p53. We and others found that Wee1 inhibition sensitizes leukemia cells to cytarabine. Thus, we sought to determine whether chemosensitization by Wee1 inhibition is dependent on p53 dysfunction and whether combining Wee1 inhibition is tolerable and effective in vi  ...[more]

Similar Datasets

Unknown WEE1 inhibition sensitizes osteosarcoma to radiotherapy.
| S-EPMC3103478 | biostudies-literature
Unknown STAT3 inhibition sensitizes colorectal cancer to chemoradiotherapy in vitro and in vivo.
| S-EPMC7706351 | biostudies-literature
Unknown Cyclin E Overexpression Sensitizes Triple-Negative Breast Cancer to Wee1 Kinase Inhibition.
| S-EPMC6317865 | biostudies-literature
Unknown Prolonged mitotic arrest induced by Wee1 inhibition sensitizes breast cancer cells to paclitaxel.
| S-EPMC5650293 | biostudies-literature
Transcriptomics Wee1 Inhibition sensitizes prostate cancer cells to Hsp90 inhibitor to activate the intrinsic apoptotic pathway
2013-01-10 | E-GEOD-38972 | biostudies-arrayexpress
Unknown Wee1 inhibition potentiates Wip1-dependent p53-negative tumor cell death during chemotherapy.
| S-EPMC4855675 | biostudies-literature
Transcriptomics Inhibition of the mRNA-binding protein IGF2BP1 suppresses proliferation and sensitizes neuroblastoma cells to chemotherapeutics
2021-04-07 | GSE158258 | GEO
Unknown Daxx Functions Are p53-Independent In Vivo.
| S-EPMC6233723 | biostudies-literature
Unknown p53-independent p21 induction by MELK inhibition.
| S-EPMC5601624 | biostudies-literature
Unknown ATM kinase inhibition preferentially sensitizes p53-mutant glioma to ionizing radiation.
| S-EPMC3687028 | biostudies-literature