Inefficient recruitment of DDX39B impedes prespliceosome assembly on FOXP3 introns

Chloe K. Nagasawa, Aaron O. Bailey, William K. Russell, Mariano Garcia-Blanco

Research output: Contribution to journalArticlepeer-review

Abstract

Forkhead box P3 (FOXP3) is the master fate-determining transcription factor in regulatory T (Treg) cells and is essential for their development, function, and homeostasis. Mutations in FOXP3 cause immunodysregulation polyendocrinopathy enteropathy X-linked (IPEX) syndrome, and aberrant expression of FOXP3 has been implicated in other diseases such as multiple sclerosis and cancer. We previously demonstrated that pre-mRNA splicing of FOXP3 RNAs is highly sensitive to levels of DExD-box polypeptide 39B (DDX39B), and here we investigate the mechanism of this sensitivity. FOXP3 introns have cytidine (C)-rich/uridine (U)-poor polypyrimidine (py) tracts that are responsible for their inefficient splicing and confer sensitivity to DDX39B. We show that there is a deficiency in the assembly of commitment complexes (CCs) on FOXP3 introns, which is consistent with the lower affinity of U2AF2 for C-rich/U-poor py tracts. Our data indicate an even stronger effect on the conversion of CCs to pre-spliceosomes. We propose that this is due to an altered conformation that U2AF2 adopts when it binds to C-rich/U-poor py tracts and that this conformation has a lower affinity for DDX39B. As a consequence, CCs assembled on FOXP3 introns are defective in recruiting DDX39B, and this leads to the inefficient assembly of pre-spliceosome complexes.

Original languageEnglish (US)
Pages (from-to)824-838
Number of pages15
JournalRNA
Volume30
Issue number7
DOIs
StatePublished - Jul 2024

Keywords

  • autoimmunity
  • DDX39B
  • FOXP3
  • IPEX syndrome
  • multiple sclerosis
  • pre-mRNA splicing

ASJC Scopus subject areas

  • Molecular Biology

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