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P53-mediated delayed NF-?B activity enhances etoposide-induced cell death in medulloblastoma.


ABSTRACT: Medulloblastoma (MB) is an embryonic brain tumour that arises in the cerebellum. Using several MB cell lines, we have demonstrated that the chemotherapeutic drug etoposide induces a p53- and caspase-dependent cell death. We have observed an additional caspase-independent cell death mechanism involving delayed nuclear factor ?B (NF-?B) activity. The delayed induction was controlled by a p53-dependent transcription step and the production of death receptors (especially CD95/Fas). We further demonstrated that in both MB and glioblastoma (GM) cell lines, in which the p53 pathway was not functional, no p65 activation could be detected upon etoposide treatment. MB cell lines that have mutations in p53 or NF-?B are either less sensitive (NF-?B mutant) or even completely resistant (p53 mutant) to chemotherapeutic intervention. The optimal cell death was only achieved when both p53 and NF-?B were switched on. Taken together, our results shed light on the mechanism of NF-?B activation by etoposide in brain tumours and show that the genetic background of MB and GM cells determines their sensitivity to chemotherapy and has to be taken into account for efficient therapeutic intervention.

SUBMITTER: Meley D 

PROVIDER: S-EPMC3032310 | biostudies-literature | 2010 May

REPOSITORIES: biostudies-literature

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p53-mediated delayed NF-κB activity enhances etoposide-induced cell death in medulloblastoma.

Meley D D   Spiller D G DG   White M R H MR   McDowell H H   Pizer B B   Sée V V  

Cell death & disease 20100513


Medulloblastoma (MB) is an embryonic brain tumour that arises in the cerebellum. Using several MB cell lines, we have demonstrated that the chemotherapeutic drug etoposide induces a p53- and caspase-dependent cell death. We have observed an additional caspase-independent cell death mechanism involving delayed nuclear factor κB (NF-κB) activity. The delayed induction was controlled by a p53-dependent transcription step and the production of death receptors (especially CD95/Fas). We further demons  ...[more]

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