Active eosinophils regulate host defence and immune responses in colitis

Alessandra Gurtner(University of Zurich), Costanza Borrelli(ETH Zurich), Ignacio Gonzalez-Perez(University of Zurich), Karsten Bach(ETH Zurich), İlhan E. Acar(ETH Zurich), Nicolás Gonzalo Núñez(University of Zurich), Daniel Crepaz(University of Zurich), Kristina Handler(ETH Zurich), Vivian Vu(University of Bern), Atefeh Lafzi(ETH Zurich), Kristin Stirm(University of Zurich), Deeksha Raju(University of Zurich), Julia Gschwend(University of Zurich), Konrad Basler(University of Zurich), Christoph Schneider(University of Zurich), Emma Slack(ETH Zurich), Tomáš Valenta(University of Zurich), Burkhard Becher(University of Zurich), Philippe Krebs(University of Bern), Andreas E. Moor(ETH Zurich), Isabelle C. Arnold(University of Zurich)
Nature
December 12, 2022
Cited by 163Open Access
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Abstract

Abstract In the past decade, single-cell transcriptomics has helped to uncover new cell types and states and led to the construction of a cellular compendium of health and disease. Despite this progress, some difficult-to-sequence cells remain absent from tissue atlases. Eosinophils—elusive granulocytes that are implicated in a plethora of human pathologies 1–5 —are among these uncharted cell types. The heterogeneity of eosinophils and the gene programs that underpin their pleiotropic functions remain poorly understood. Here we provide a comprehensive single-cell transcriptomic profiling of mouse eosinophils. We identify an active and a basal population of intestinal eosinophils, which differ in their transcriptome, surface proteome and spatial localization. By means of a genome-wide CRISPR inhibition screen and functional assays, we reveal a mechanism by which interleukin-33 (IL-33) and interferon-γ (IFNγ) induce the accumulation of active eosinophils in the inflamed colon. Active eosinophils are endowed with bactericidal and T cell regulatory activity, and express the co-stimulatory molecules CD80 and PD-L1. Notably, active eosinophils are enriched in the lamina propria of a small cohort of patients with inflammatory bowel disease, and are closely associated with CD4 + T cells. Our findings provide insights into the biology of eosinophils and highlight the crucial contribution of this cell type to intestinal homeostasis, immune regulation and host defence. Furthermore, we lay a framework for the characterization of eosinophils in human gastrointestinal diseases.


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