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Interferon-responsive intestinal BEST4/CA7+ cells are targets of bacterial diarrheal toxins

  • Daisong Wang
  • , Willem Kasper Spoelstra
  • , Lin Lin
  • , Ninouk Akkerman
  • , Daniel Krueger
  • , Talya Dayton
  • , Jeroen S. van Zon
  • , Sander J. Tans
  • , Johan H. van Es
  • , Hans Clevers

Research output: Contribution to journalArticlepeer-review

14 Citations (Scopus)

Abstract

BEST4/CA7+ cells of the human intestine were recently identified by single-cell RNA sequencing. While their gene expression profile predicts a role in electrolyte balance, BEST4/CA7+ cell function has not been explored experimentally owing to the absence of BEST4/CA7+ cells in mice and the paucity of human in vitro models. Here, we establish a protocol that allows the emergence of BEST4/CA7+ cells in human intestinal organoids. Differentiation of BEST4/CA7+ cells requires activation of Notch signaling and the transcription factor SPIB. BEST4/CA7+ cell numbers strongly increase in response to the cytokine interferon-γ, supporting a role in immunity. Indeed, we demonstrate that BEST4/CA7+ cells generate robust CFTR-mediated fluid efflux when stimulated with bacterial diarrhea-causing toxins and find the norepinephrine-ADRA2A axis as a potential mechanism in blocking BEST4/CA7+ cell-mediated fluid secretion. Our observations identify a central role of BEST4/CA7+ cells in fluid homeostasis in response to bacterial infections.

Original languageEnglish
Pages (from-to)598-612.e5
JournalCell stem cell
Volume32
Issue number4
DOIs
Publication statusPublished - 3 Apr 2025

Keywords

  • BEST4/CA7 cells
  • bacterial infection
  • fluid homeostasis
  • human intestinal organoids
  • interferon-γ
  • Cell Differentiation/drug effects
  • Humans
  • Interferon-gamma/pharmacology
  • Diarrhea/microbiology
  • Bacterial Toxins/toxicity
  • Interferons/pharmacology
  • Organoids/metabolism
  • Signal Transduction/drug effects
  • Animals
  • Intestines/cytology
  • Mice

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