Nature Communications (Dec 2024)

The capicua-ataxin-1-like complex regulates Notch-driven marginal zone B cell development and sepsis progression

  • Jong Seok Park,
  • Minjung Kang,
  • Han Bit Kim,
  • Hyebeen Hong,
  • Jongeun Lee,
  • Youngkwon Song,
  • Yunjung Hur,
  • Soeun Kim,
  • Tae-Kyung Kim,
  • Yoontae Lee

DOI
https://doi.org/10.1038/s41467-024-54803-z
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 15

Abstract

Read online

Abstract Follicular B (FOB) and marginal zone B (MZB) cells are pivotal in humoral immune responses against pathogenic infections. MZB cells can exacerbate endotoxic shock via interleukin-6 secretion. Here we show that the transcriptional repressor capicua (CIC) and its binding partner, ataxin-1-like (ATXN1L), play important roles in FOB and MZB cell development. CIC deficiency reduces the size of both FOB and MZB cell populations, whereas ATXN1L deficiency specifically affects MZB cells. B cell receptor signaling is impaired only in Cic-deficient FOB cells, whereas Notch signaling is disrupted in both Cic-deficient and Atxn1l-deficient MZB cells. Mechanistically, ETV4 de-repression leads to inhibition of Notch1 and Notch2 transcription, thereby inhibiting MZB cell development in B cell-specific Cic-deficient (Cic f/f ;Cd19-Cre) and Atxn1l-deficient (Atxn1l f/f ;Cd19-Cre) mice. In Cic f/f ;Cd19-Cre and Atxn1l f/f ; Cd19-Cre mice, humoral immune responses and lipopolysaccharide-induced sepsis progression are attenuated but are restored upon Etv4-deletion. These findings highlight the importance of the CIC-ATXN1L complex in MZB cell development and may provide proof of principle for therapeutic targeting in sepsis.