Please use this identifier to cite or link to this item:http://hdl.handle.net/20.500.12105/8879
Title
Lamin A/C deficiency in CD4+ T-cells enhances regulatory T-cells and prevents inflammatory bowel disease
Author(s)
Toribio-Fernandez, Raquel CNIC | Herrero-Fernandez, Beatriz CNIC | Zorita, Virginia CNIC | Lopez, Juan Antonio CNIC | Vazquez, Jesus CNIC | Criado, Gabriel | Pablos, Jose L | Collas, Philippe | Sanchez-Madrid, Francisco CNIC | Andres, Vicente CNIC | Gonzalez-Granado, Jose Maria CNIC
Date issued
2019-12
Citation
J Pathol. 2019; 249(4):509-22
Language
Inglés
Document type
journal article
Abstract
The mechanisms by which lamin A/C in CD4+ T-cells control intestinal homeostasis and can cause inflammatory bowel disease (IBD) are unknown. Here, we explore lamin A/C in a mouse model of IBD. Adoptive transfer to Rag1-/- mice of Lmna-/- CD4+ T-cells, which have enhanced regulatory T-cells (Treg) differentiation and function, induced less severe IBD than wild-type T-cells. Lamin A/C deficiency in CD4+ T-cells enhanced transcription of the Treg master regulator FOXP3, thus promoting Treg differentiation, and reduced Th1 polarization, due to epigenetic changes in the Th1 master regulator T-bet. In mesenteric lymph nodes, retinoic acid (RA) released by CD103+ dendritic cells downregulated lamin A/C in CD4+ T-cells, enhancing Treg differentiation. However, non-RA-producing CD103- dendritic cells predominated in peripheral lymph nodes, facilitating lamin A/C expression in CD4+ T-cells and therefore Th1 differentiation. Our findings establish lamin A/C as a key regulator of Th differentiation in physiological conditions and show it as a potential immune-regulatory target in IBD. © 2019 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.
Subject
DOI
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