CNBP controls IL-12 gene transcription and Th1 immunity.
Yongzhi ChenShruti SharmaPatricia A AssisZhaozhao JiangRoland EllingAndrew J OliveSaiyu HangJennifer BernierJun R HuhChristopher M SassettiDavid M KnipeRicardo T GazzinelliKatherine A FitzgeraldPublished in: The Journal of experimental medicine (2018)
An inducible program of inflammatory gene expression is a hallmark of antimicrobial defenses. Recently, cellular nucleic acid-binding protein (CNBP) was identified as a regulator of nuclear factor-kappaB (NF-κB)-dependent proinflammatory cytokine gene expression. Here, we generated mice lacking CNBP and found that CNBP regulates a very restricted gene signature that includes IL-12β. CNBP resides in the cytosol of macrophages and translocates to the nucleus in response to diverse microbial pathogens and pathogen-derived products. Cnbp-deficient macrophages induced canonical NF-κB/Rel signaling normally but were impaired in their ability to control the activation of c-Rel, a key driver of IL-12β gene transcription. The nuclear translocation and DNA-binding activity of c-Rel required CNBP. Lastly, Cnbp-deficient mice were more susceptible to acute toxoplasmosis associated with reduced production of IL-12β, as well as a reduced T helper type 1 (Th1) cell IFN-γ response essential to controlling parasite replication. Collectively, these findings identify CNBP as important regulator of c-Rel-dependent IL-12β gene transcription and Th1 immunity.
Keyphrases
- gene expression
- nuclear factor
- transcription factor
- dna binding
- genome wide
- copy number
- genome wide identification
- dna methylation
- signaling pathway
- nucleic acid
- binding protein
- immune response
- liver failure
- staphylococcus aureus
- single cell
- microbial community
- intensive care unit
- candida albicans
- cell therapy
- inflammatory response
- drug induced
- endothelial cells