NF-κB/p52 augments ETS1 binding genome-wide to promote glioma progression.
Nicholas SimYinghui LiPublished in: Communications biology (2023)
Gliomas are highly invasive and chemoresistant cancers, making them challenging to treat. Chronic inflammation is a key driver of glioma progression as it promotes aberrant activation of inflammatory pathways such as NF-κB signalling, which drives cancer cell invasion and angiogenesis. NF-κB factors typically dimerise with its own family members, but emerging evidence of their promiscuous interactions with other oncogenic factors has been reported to promote transcription of new target genes and function. Here, we show that non-canonical NF-κB activation directly regulates p52 at the ETS1 promoter, activating its expression. This impacts the genomic and transcriptional landscape of ETS1 in a glioma-specific manner. We further show that enhanced non-canonical NF-κB signalling promotes the co-localisation of p52 and ETS1, resulting in transcriptional activation of non-κB and/or non-ETS glioma-promoting genes. We conclude that p52-induced ETS1 overexpression in glioma cells remodels the genome-wide regulatory network of p52 and ETS1 to transcriptionally drive cancer progression.
Keyphrases
- transcription factor
- genome wide
- signaling pathway
- oxidative stress
- genome wide identification
- lps induced
- dna binding
- pi k akt
- dna methylation
- nuclear factor
- papillary thyroid
- copy number
- gene expression
- squamous cell
- diabetic rats
- poor prognosis
- endothelial cells
- inflammatory response
- cell proliferation
- immune response
- young adults
- squamous cell carcinoma
- toll like receptor
- drug induced
- high glucose
- lymph node metastasis
- genome wide analysis