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BCL6 is a context-dependent mediator of the glioblastoma response to irradiation therapy

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posted on 2025-02-26, 20:52 authored by AKW Tribe, Lifeng PengLifeng Peng, Paul Teesdale-SpittlePaul Teesdale-Spittle, Melanie-Jane McConnellMelanie-Jane McConnell
Glioblastoma is a rapidly fatal brain cancer that does not respond to therapy. Previous research showed that the transcriptional repressor protein BCL6 is upregulated by chemo and radiotherapy in glioblastoma, and inhibition of BCL6 enhances the effectiveness of these therapies. Therefore, BCL6 is a promising target to improve the efficacy of current glioblastoma treatment. BCL6 acts as a transcriptional repressor in germinal centre B cells and as an oncogene in lymphoma and other cancers. However, in glioblastoma, BCL6 induced by therapy may not be able to repress transcription. Using a BCL6 inhibitor, the whole proteome response to irradiation was compared with and without BCL6 activity. Acute high dose irradiation caused BCL6 to switch from repressing the DNA damage response to promoting stress response signalling. Rapid immunoprecipitation mass spectrometry of endogenous proteins (RIME) enabled comparison of BCL6 partner proteins between untreated and irradiated glioblastoma cells. BCL6 was associated with transcriptional coregulators in untreated glioblastoma including the known partner NCOR2. However, this association was lost in response to acute irradiation, where BCL6 unexpectedly associated with synaptic and plasma membrane proteins. These results reveal the activity of BCL6 under therapy-induced stress is context-dependent, and potentially altered by the intensity of that stress.

History

Preferred citation

Tribe, A. K. W., Peng, L., Teesdale-Spittle, P. H. & McConnell, M. J. (2024). BCL6 is a context-dependent mediator of the glioblastoma response to irradiation therapy. International Journal of Biological Macromolecules, 270(Pt 1), 131782-131782. https://doi.org/10.1016/j.ijbiomac.2024.131782

Journal title

International Journal of Biological Macromolecules

Volume

270

Issue

Pt 1

Publication date

2024-06-01

Pagination

131782-131782

Publisher

Elsevier BV

Publication status

Published

Online publication date

2024-05-10

ISSN

0141-8130

eISSN

1879-0003

Article number

131782

Language

en