串扰
肝细胞
免疫
细胞生物学
巨噬细胞
生物
化学
免疫系统
免疫学
遗传学
物理
光学
体外
作者
Wei Liang Gan,Xi Ren,Vanessa Hui En Ng,Larry Ng,Yangyang Song,Vincent Tano,Jian Han,Ömer An,Jinghe Xie,Bryan Yik Loong Ng,Daryl Jin Tai Tay,Sze Jing Tang,Haoqing Shen,Shruti Khare,Kelvin Han Chung Chong,Yock Young Dan,Bin Wu,Ramanuj DasGupta,Leilei Chen
出处
期刊:Cell Reports
[Elsevier]
日期:2024-06-26
卷期号:43 (7): 114400-114400
标识
DOI:10.1016/j.celrep.2024.114400
摘要
ADAR1-mediated RNA editing establishes immune tolerance to endogenous double-stranded RNA (dsRNA) by preventing its sensing, primarily by MDA5. Although deleting Ifih1 (encoding MDA5) rescues embryonic lethality in ADAR1-deficient mice, they still experience early postnatal death, and removing other MDA5 signaling proteins does not yield the same rescue. Here, we show that ablation of MDA5 in a liver-specific Adar knockout (KO) murine model fails to rescue hepatic abnormalities caused by ADAR1 loss. Ifih1;Adar double KO (dKO) hepatocytes accumulate endogenous dsRNAs, leading to aberrant transition to a highly inflammatory state and recruitment of macrophages into dKO livers. Mechanistically, progranulin (PGRN) appears to mediate ADAR1 deficiency-induced liver pathology, promoting interferon signaling and attracting epidermal growth factor receptor (EGFR)+ macrophages into dKO liver, exacerbating hepatic inflammation. Notably, the PGRN-EGFR crosstalk communication and consequent immune responses are significantly repressed in ADAR1high tumors, revealing that pre-neoplastic or neoplastic cells can exploit ADAR1-dependent immune tolerance to facilitate immune evasion.
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