Human gut M cells resemble dendritic cells and present gluten antigen

Journal Article (2025)
Author(s)

Daisong Wang (University Medical Center Utrecht)

Willine J. van de Wetering (Maastricht University)

Yuu Okura (Chugai Pharmaceutical)

Gijs J.F. van Son (Princess Máxima Center for Pediatric Oncology)

Apollo Pronk (Diakonessehuis Utrecht)

Gieneke B.C. Gonera-de Jong (Wilhelmina Hospital Assen)

Sebo Withoff (University Medical Center Groningen)

Sander J. Tans (AMOLF Institute for Atomic and Molecular Physics, TU Delft - BN/Sander Tans Lab, Kavli institute of nanoscience Delft)

Peter J. Peters (Maastricht University)

Hans Clevers (Oncode Institute, Roche Innovation Center, University Medical Center Utrecht)

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Research Group
BN/Sander Tans Lab
DOI related publication
https://doi.org/10.1038/s41586-025-09829-8
More Info
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Publication Year
2025
Language
English
Research Group
BN/Sander Tans Lab
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Abstract

Microfold (M) cells are rare intestinal epithelial cells that reside in the follicle-associated epithelium of Peyer’s patches1. M cells transport luminal antigens to submucosal antigen-presenting cells2,3. These insights primarily derive from transmission electron microscopy and studies using genetically modified mice2, 3–4. Here we establish an intestinal organoid model to study human M cells and reconstruct the differentiation trajectory of M cells through transcriptome profiling. The results indicate that as well as facilitating luminal antigen transport, human M cells also directly present antigens via the class II major histocompatibility complex (MHC-II). Notably, the related enterocytes only express MHC-II in chronic inflammatory states and do not express typical dendritic cell markers. Human M cells physiologically express a gene profile that resembles that of dendritic cells. Similar to dendritic cells, M cell development is induced by RANKL and CSF2 and requires the transcription factors SPIB and RUNX2. HLA-DQ2.5 M cells process and present gluten antigen as demonstrated in organoid–T cell co-culture assays. These findings suggest that M cells may have a central role in coeliac disease.