Rapid P-TEFb-dependent transcriptional reorganization underpins the glioma adaptive response to radiotherapy.
Faye M WalkerLays Martin SobralEtienne DanisBridget SanfordSahiti DonthulaIlango BalakrishnanDong WangAngela PierceSana D KaramSoudabeh KargarNatalie J SerkovaNicholas K ForemanSujatha VenkataramanRobin D DowellRajeev VibhakarNathan A DahlPublished in: Nature communications (2024)
Dynamic regulation of gene expression is fundamental for cellular adaptation to exogenous stressors. P-TEFb-mediated pause-release of RNA polymerase II (Pol II) is a conserved regulatory mechanism for synchronous transcriptional induction in response to heat shock, but this pro-survival role has not been examined in the applied context of cancer therapy. Using model systems of pediatric high-grade glioma, we show that rapid genome-wide reorganization of active chromatin facilitates P-TEFb-mediated nascent transcriptional induction within hours of exposure to therapeutic ionizing radiation. Concurrent inhibition of P-TEFb disrupts this chromatin reorganization and blunts transcriptional induction, abrogating key adaptive programs such as DNA damage repair and cell cycle regulation. This combination demonstrates a potent, synergistic therapeutic potential agnostic of glioma subtype, leading to a marked induction of tumor cell apoptosis and prolongation of xenograft survival. These studies reveal a central role for P-TEFb underpinning the early adaptive response to radiotherapy, opening avenues for combinatorial treatment in these lethal malignancies.
Keyphrases
- gene expression
- transcription factor
- heat shock
- genome wide
- cell cycle
- dna damage
- dna methylation
- cancer therapy
- high grade
- cell proliferation
- early stage
- locally advanced
- oxidative stress
- heat stress
- radiation therapy
- heat shock protein
- dna repair
- radiation induced
- anti inflammatory
- squamous cell carcinoma
- loop mediated isothermal amplification
- free survival
- low grade
- replacement therapy