The immune-epithelial-stromal interactions underpinning intestinal damage in celiac disease (CD) are incompletely understood. To address this, we performed single-cell transcriptomics (RNA sequencing; 86,442 immune, parenchymal and epithelial cells; 35 participants) and spatial transcriptomics (20 participants) on CD intestinal biopsy samples. Here we show that in CD, epithelial populations shifted toward a progenitor state, with interferon-driven transcriptional responses, and perturbation of secretory and enteroendocrine populations. Mucosal T cells showed numeric and functional changes in regulatory and follicular helper-like CD4(+) T cells, intraepithelial lymphocytes, CD8(+) and γδ T cell subsets, with skewed T cell antigen receptor repertoires. Mucosal changes remained detectable despite treatment, representing a persistent immune-epithelial 'scar'. Spatial transcriptomics defined transcriptional niches beyond those captured in conventional histological scores, including CD-specific lymphoid aggregates containing T cell-B cell interactions. Receptor-ligand spatial analyses integrated with disease susceptibility gene expression defined networks of altered chemokine and morphogen signaling, and provide potential therapeutic targets for CD prevention and treatment.
Immune-epithelial-stromal networks define the cellular ecosystem of the small intestine in celiac disease.
免疫-上皮-基质网络定义了乳糜泻小肠的细胞生态系统
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作者:FitzPatrick Michael E B, Antanaviciute Agne, Dunstan Melanie, Künnapuu Karolina, Trzupek Dominik, Provine Nicholas M, Dooley Kyla, Zhang Jia-Yuan, Irwin Sophie L, Garner Lucy C, Pernes Jane I, Ferreira Ricardo C, Sasson Sarah C, Aschenbrenner Dominik, Agarwal Devika, Rodrigues Astor, Howarth Lucy, Brain Oliver, Ruane Darren, Soilleux Elizabeth, Teichmann Sarah A, Dendrou Calliope A, Simmons Alison, Uhlig Holm H, Todd John A, Klenerman Paul
| 期刊: | Nature Immunology | 影响因子: | 27.600 |
| 时间: | 2025 | 起止号: | 2025 Jun;26(6):947-962 |
| doi: | 10.1038/s41590-025-02146-2 | 研究方向: | 细胞生物学 |
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