肥大细胞
转录组
细胞
生物
计算生物学
细胞生物学
遗传学
免疫学
基因
基因表达
作者
Hind Hussein,Elodie Modave,Nathalie Stakenborg,Marcello Delfini,Katy Vandereyken,Alejandro Sifrim,Thierry Voet,Guy E. Boeckxstaens
出处
期刊:
[Cold Spring Harbor Laboratory]
日期:2024-12-03
被引量:2
标识
DOI:10.1101/2024.11.29.626054
摘要
Abstract Gut mast cells are key players in infection and inflammation, as well as in homeostasis. Mast cells regulate gastrointestinal (GI) function by controlling vascular and epithelial permeability, and interacting with the immune system and the enteric nervous system. Mucosal (MC T ) and connective tissue (MC TC ) mast cells coexist in the gastrointestinal tract, but are located in distinct microanatomical niches. However, little is known about the transcriptional heterogeneity of human intestinal mast cells. Additionally, whether distinct microanatomical niches instruct mast cell phenotypes in the human gut is currently unknown. We therefore performed 10x single cell RNA sequencing on healthy rectal biopsies and on dissected layers of human sigmoid colon. We identified five transcriptionally distinct mast cell subsets (MC1-5) which exhibited a layer-specific distribution in the healthy human colon and distinct cytokine, chemokine, protease, and transcription factor profiles, and were associated with putative immune and neuro-immune functions. This study provides a framework for the integration of mast cell heterogeneity in the study of gastrointestinal disease mechanisms in humans.
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