Communications Biology (May 2024)

E4BP4 in macrophages induces an anti-inflammatory phenotype that ameliorates the severity of colitis

  • Yasuko Kajimura,
  • Akihiko Taguchi,
  • Yuko Nagao,
  • Kaoru Yamamoto,
  • Konosuke Masuda,
  • Kensuke Shibata,
  • Yoichi Asaoka,
  • Makoto Furutani-Seiki,
  • Yukio Tanizawa,
  • Yasuharu Ohta

DOI
https://doi.org/10.1038/s42003-024-06099-4
Journal volume & issue
Vol. 7, no. 1
pp. 1 – 13

Abstract

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Abstract Macrophages are versatile cells of the innate immune system that work by altering their pro- or anti-inflammatory features. Their dysregulation leads to inflammatory disorders such as inflammatory bowel disease. We show that macrophage-specific upregulation of the clock output gene and transcription factor E4BP4 reduces the severity of colitis in mice. RNA-sequencing and single-cell analyses of macrophages revealed that increased expression of E4BP4 leads to an overall increase in expression of anti-inflammatory genes including Il4ra with a concomitant reduction in pro-inflammatory gene expression. In contrast, knockout of E4BP4 in macrophages leads to increased proinflammatory gene expression and decreased expression of anti-inflammatory genes. ChIP-seq and ATAC-seq analyses further identified Il4ra as a target of E4BP4, which drives anti-inflammatory polarization in macrophages. Together, these results reveal a critical role for E4BP4 in regulating macrophage inflammatory phenotypes and resolving inflammatory bowel diseases.