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Radiotherapy followed by aurora kinase inhibition targets tumor-propagating cells in human glioblastoma.


ABSTRACT: Glioblastoma (GBM) is the most common malignant primary brain tumor. Radiotherapy fails to eliminate subpopulations of stem-like tumor-propagating cells (TPC), resulting in tumor regrowth. To identify kinases that promote TPC self-renewal rather than increasing proliferation in human GBM cultures, we screened a library of 54 nonselective tool compounds and determined their kinase inhibitor profiles in vitro. Most compounds inhibited aurora kinase (AURK) activity and blocked TPC self-renewal, while inducing GBM cell polynucleation and apoptosis. To prevent regrowth by TPCs, we used a priming dose of radiation followed by incubation with the pan-AURK inhibitor VX680 to block self-renewal and induce apoptosis in GBM cultures. In mice xenografted with human GBM cells, radiotherapy followed by VX680 treatment resulted in reduced tumor growth and increased survival relative to either monotherapy alone or VX680 treatment before radiation. Our results indicate that AURK inhibition, subsequent to radiation, may enhance the efficacy of radiotherapy by targeting radioresistant TPCs in human GBMs.

SUBMITTER: Li N 

PROVIDER: S-EPMC4326592 | biostudies-literature | 2015 Feb

REPOSITORIES: biostudies-literature

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Radiotherapy followed by aurora kinase inhibition targets tumor-propagating cells in human glioblastoma.

Li Nan N   Maly Dustin J DJ   Chanthery Yvan H YH   Sirkis Daniel W DW   Nakamura Jean L JL   Berger Mitchel S MS   James C David CD   Shokat Kevan M KM   Weiss William A WA   Persson Anders I AI  

Molecular cancer therapeutics 20141218 2


Glioblastoma (GBM) is the most common malignant primary brain tumor. Radiotherapy fails to eliminate subpopulations of stem-like tumor-propagating cells (TPC), resulting in tumor regrowth. To identify kinases that promote TPC self-renewal rather than increasing proliferation in human GBM cultures, we screened a library of 54 nonselective tool compounds and determined their kinase inhibitor profiles in vitro. Most compounds inhibited aurora kinase (AURK) activity and blocked TPC self-renewal, whi  ...[more]

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