Histone demethylase JMJD1A protects mice from enteric bacterial infection by upregulating CCL8 expression to recruit macrophages and CD4+ T cells
Guifang Lin, Lichun Yang, Shuyan Jiang, Yong Zhang, Ping Luo, Weihua Li, Jianming Xu, Gongpeng Xiong, Chundong Yu, Wenbo Chen, George Deepe, George Deepe, George Deepe

TL;DR
This study shows that the histone demethylase JMJD1A helps protect mice from gut bacterial infections by boosting CCL8, which attracts immune cells to fight the infection.
Contribution
The study reveals a novel role of JMJD1A in host defense against enteric bacterial infection through CCL8 upregulation.
Findings
JMJD1A-/- mice showed increased mortality and colonic injury after C. rodentium infection.
CCL8 expression was reduced in JMJD1A-/- mice, impairing macrophage and CD4+ T cell recruitment.
JMJD1A promotes CCL8 expression by demethylating H3K9me2 on its promoter in collaboration with IRF1.
Abstract
Jumonji domain-containing 1A (JMJD1A, also known as KDM3A) is a histone demethylase that specifically demethylates H3K9me1/2 to enhance gene expression. The roles of JMJD1A in many physiological and pathological processes have been revealed. However, it is unclear whether JMJD1A is involved in host defense against enteric pathogen infection. In this study, we found that enteric infection with C. rodentium induced JMJD1A expression in colonic epithelial cells at the transcriptional level partly mediated by IRF1. After C. rodentium infection, JMJD1A-/- mice exhibited increased mortality, colonic injury, and C. rodentium load and systemic spread, suggesting that JMJD1A protects host against C. rodentium infection by enhancing C. rodentium clearance. JMJD1A-/- mice exhibited an impaired colonic recruitment of macrophages and CD4+ T cells as well as a reduced production of C.…
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Taxonomy
TopicsGut microbiota and health · Epigenetics and DNA Methylation · Immune cells in cancer
