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Oncotarget

GBP3-STING Interaction in Glioblastoma Coordinates Poor Response to Temozolomide

Oct 17, 2023
This podcast discusses the challenges of temozolomide treatment for glioblastoma and the role of the GBP3-STING interaction in the development and recurrence of this tumor. It explores the impact of GBP3 upregulation on temozolomide response, which is associated with worse survival outcomes.
03:33

Podcast summary created with Snipd AI

Quick takeaways

  • GBP3 plays a pro-tumor role in Glioblastoma and its high expression is linked to resistance to Temizolomide treatment.
  • Diverse reactions to Temizolomide in Glioblastoma hinder further progress, but understanding the role of GBP3 can open avenues for targeted therapies.

Deep dives

GBP3 Sting Interaction in Glioblastoma Coordinates Autophagy, Antioxidative, and DNA Repair Programs

The recent editorial paper published in Onco Targets Vol. 14 discusses the role of GBP3 in Glioblastoma development and recurrence. GBP family members, including GBP3, play pro-tumor roles and are highly elevated in Glioblastoma. GBP3 specifically shows significant upregulation in response to Temizolomide, the standard adjuvant chemotherapeutic drug for Glioblastoma. High levels of GBP3 expression are associated with worse overall survival after Temizolomide treatment. Exogenous expression of GBP3 induced Temizolomide resistance, while GBP3 silencing conferred Temizolomide sensitivity both in vitro and in vivo. This resistance is linked to the accumulation of cytoplasmic DNA fragments, suggesting the involvement of Stimulator of Interferon Genes (STING).

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