Login / Signup

Disrupting the phase separation of KAT8-IRF1 diminishes PD-L1 expression and promotes antitumor immunity.

Yuanzhong WuLiwen ZhouYezi ZouYijun ZhangMeifang ZhangLiping XuLisi ZhengWenting HeKuai YuTing LiXia ZhangZhenxuan ChenRuhua ZhangPenghui ZhouNu ZhangLimin ZhengTie-Bang Kang
Published in: Nature cancer (2023)
Immunotherapies targeting the PD-1/PD-L1 axis have become first-line treatments in multiple cancers. However, only a limited subset of individuals achieves durable benefits because of the elusive mechanisms regulating PD-1/PD-L1. Here, we report that in cells exposed to interferon-γ (IFNγ), KAT8 undergoes phase separation with induced IRF1 and forms biomolecular condensates to upregulate PD-L1. Multivalency from both the specific and promiscuous interactions between IRF1 and KAT8 is required for condensate formation. KAT8-IRF1 condensation promotes IRF1 K78 acetylation and binding to the CD247 (PD-L1) promoter and further enriches the transcription apparatus to promote transcription of PD-L1 mRNA. Based on the mechanism of KAT8-IRF1 condensate formation, we identified the 2142-R8 blocking peptide, which disrupts KAT8-IRF1 condensate formation and consequently inhibits PD-L1 expression and enhances antitumor immunity in vitro and in vivo. Our findings reveal a key role of KAT8-IRF1 condensates in PD-L1 regulation and provide a competitive peptide to enhance antitumor immune responses.
Keyphrases
  • dendritic cells
  • immune response
  • transcription factor
  • dna methylation
  • induced apoptosis
  • young adults
  • oxidative stress
  • single cell
  • cancer therapy
  • inflammatory response
  • drug induced