Sumoylation coordinates the repression of inflammatory and anti-viral gene-expression programs during innate sensing.
Adrien DecqueOlivier JoffreJoao G MagalhaesJack-Christophe CossecRonnie Blecher-GonenPierre LapaquetteAymeric SilvinNicolas ManelPierre-Emmanuel JoubertJacob-Sebastian SeelerMatthew L AlbertIdo AmitSebastian AmigorenaAnne DejeanPublished in: Nature immunology (2015)
Innate sensing of pathogens initiates inflammatory cytokine responses that need to be tightly controlled. We found here that after engagement of Toll-like receptors (TLRs) in myeloid cells, deficient sumoylation caused increased secretion of transcription factor NF-κB-dependent inflammatory cytokines and a massive type I interferon signature. In mice, diminished sumoylation conferred susceptibility to endotoxin shock and resistance to viral infection. Overproduction of several NF-κB-dependent inflammatory cytokines required expression of the type I interferon receptor, which identified type I interferon as a central sumoylation-controlled hub for inflammation. Mechanistically, the small ubiquitin-like modifier SUMO operated from a distal enhancer of the gene encoding interferon-β (Ifnb1) to silence both basal and stimulus-induced activity of the Ifnb1 promoter. Therefore, sumoylation restrained inflammation by silencing Ifnb1 expression and by strictly suppressing an unanticipated priming by type I interferons of the TLR-induced production of inflammatory cytokines.
Keyphrases
- oxidative stress
- dendritic cells
- immune response
- diabetic rats
- transcription factor
- gene expression
- induced apoptosis
- signaling pathway
- poor prognosis
- binding protein
- high glucose
- dna methylation
- lps induced
- nuclear factor
- toll like receptor
- public health
- acute myeloid leukemia
- pi k akt
- drug induced
- bone marrow
- small molecule
- long non coding rna
- social media
- sars cov
- dna binding
- cell death
- gram negative
- bioinformatics analysis