再生(生物学)
胎儿
炎症
细胞生物学
医学
免疫学
生物
怀孕
遗传学
作者
Antonion Korcari,Helen M. Tauc,Jeff Duggan,Fabien Wehbe,Spyros Darmanis,Zora Modrušan,Jina Yun,Rajita Pappu,David Garfield,Heinrich Jasper,David Castillo‐Azofeifa
出处
期刊:
[Cold Spring Harbor Laboratory]
日期:2025-07-19
标识
DOI:10.1101/2025.07.16.665215
摘要
Abstract Aging is associated with a decline in the regenerative capacity of many tissues. Central to this decline is a complex interplay between inflammation and stem cell function. How these two processes are linked and influence regenerative capacity remains unclear. Here, we undertake a comprehensive assessment of age-related changes in the mouse colon at single-cell resolution. A survey of immune and epithelial compartments revealed a hyperactivated inflammatory state in the colon of old mice characterized by the induction of an interferon γ (IFNγ) response signature in immune cells. This does not result in increased inflammation under homeostasis, but triggers a disproportionate inflammatory response, disrupting regeneration after challenge with the enteropathogen Citrobacter rodentium . Colons of old mice exhibit higher production of IFNγ by T and innate lymphoid cells (ILCs) that are associated with reduced Lgr5 + stem cells and decreased epithelial proliferation. Interestingly, we find aged intestinal epithelial cells to be hypersensitive to IFNγ signaling, inducing a regeneration-associated fetal-like gene expression signature that, in turn, renders these cells more sensitive to IFNγ-induced apoptosis. Our findings reveal an age-related imbalance in the interaction between the immune and epithelial compartments in the colon, priming the system for excessive inflammatory responses and the emergence of a hypersensitive epithelial cell state thus derailing proper repair of the intestinal epithelium after injury.
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