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. 2025 Jul 8:noaf160.
doi: 10.1093/neuonc/noaf160. Online ahead of print.

Proneural-Mesenchymal hybrid glioblastoma cells are resistant to therapy and dependent on nuclear import

Guillaume Bourmeau  1 Oceane Anezo  1 Jeremy Raymond  2 Alberto Ballestín  1 Cathy Pichol-Thievend  1 Juliette Reveilles  1 Adrien Thomas  1 Lin Wang  3 Melanie Miranda  4   5   6 Eve Moutaux  4   5   6 Stephane Liva  7   8 Valentino Ribecco  1 Laetitia Besse  9 Florent Dingli  10 Damarys Loew  10 Celine Vallot  4   5   6 Gaetano Gargiulo  11 Vidhya M Ravi  12   13 Kevin Joseph  12   13 Giorgio Seano  1
Affiliations

Proneural-Mesenchymal hybrid glioblastoma cells are resistant to therapy and dependent on nuclear import

Guillaume Bourmeau et al. Neuro Oncol. .

Abstract

Background: Despite extensive research efforts, glioblastoma (GBM) remains a deadly disease with poor prognosis. Although previous studies have identified various cell states within GBM tumors, the molecular mechanism underlying adaptive GBM cell plasticity induced by conventional therapy remains unclear.

Methods: We used fluorescent reporters for proneural (PN) and mesenchymal (MES) subtypes to monitor GBM cell plasticity in real-time across multiple patient-derived cell lines. This approach revealed cells that concurrently expressed both proneural and mesenchymal markers. To investigate this unique hybrid population, we implemented a comprehensive methodological approach encompassing bulk and single-cell RNA sequencing, single-cell ChIP sequencing, nuclear proteomics, high-resolution imaging, orthotopic mouse models, clinical dataset analysis, and pharmacological and genetic techniques. This multifaceted strategy allowed us to gain functional and molecular insights into this distinct cellular population.

Results: We showed that these hybrid cells are increased by conventional therapies, and are resistant to these therapies. At the molecular level, hybrid cells display significant alterations in chromatin structure and nuclear protein composition, elevated transcriptional activity, Myc activation, and improved transport between the nucleus and cytoplasm. Genetic and pharmaceutical inhibition of the nuclear import/export shuttling machinery, increased in hybrid cells, effectively suppressed adaptive GBM cell plasticity and hybrid identity, thereby enhancing the sensitivity of GBM cells to therapies.

Conclusion: Our results indicate that GBM hybrid cells play a crucial role in chemoradiation resistance. The nuclear transport machinery presents a potential therapeutic target for hybrid cells, offering a way to counteract the typical resistance to treatment observed in GBM.

Keywords: Glioblastoma; cell plasticity; hybrid; nuclear transport; resistance mechanisms.

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