免疫系统
条件基因敲除
生物
肿瘤微环境
趋化因子
肝癌
癌症研究
过继性细胞移植
T细胞
基因剔除小鼠
免疫
免疫学
信使核糖核酸
渗透(HVAC)
癌细胞
基因敲除
CXCL9型
免疫疗法
癌症
翻译(生物学)
癌症免疫疗法
细胞
先天免疫系统
肝星状细胞
肿瘤坏死因子α
细胞生长
CXCL16型
炎症
抗原
CCL18型
作者
S P Li,Xiao Zhao,T. Z. Song,Qiaoyi Chen,Yanqing Wu,Yuting Zhang,J. Chen,Yifan Wu,Bo Li,Xinyue Zhang,Zihao Dai,Lixia Xu,Ya Xie,A K C Cheng,Jianping Guo,Ming Kuang,Shuibin Lin,Zhenwei Peng,Sui Peng,Xuezhen Zeng
标识
DOI:10.1002/advs.202512528
摘要
Abstract The liver microenvironment is essential to immune surveillance and liver cancer progression. Here, the aim is to identify the role of METTL5, the 18S rRNA m 6 A methyltransferase, in regulating the liver immune microenvironment to promote cancer progression. Liver‐specific Mettl5 knockout (cKO) in mice exhibits increased immune cell infiltration, especially CD3 + and CD4 + T cells. Loss of Mettl5 inhibits intrahepatic cholangiocarcinoma (ICC) progression. By scRNA‐seq analysis, it is found that ICC from both cKO mice and human METTL5 low expression group correlates with increased CD8 + T cells but decreased macrophages, which is associated with better survival. Adoptive transfer of macrophages significantly promotes ICC progression. scRNA‐seq and scTCR‐seq analysis show that cKO mice exhibit reduced immunosuppressive Ms4a7 + C1qa + tumor‐associated macrophages (TAMs) but increased intratumoral IFN‐γ + CD8 + T cell infiltration and expansion. Mechanistically, METTL5‐mediated 18S rRNA m 6 A modification downregulates the mRNA translation of CXCL16 to exclude CD8 + T cells. Knockout of Mettl5 significantly increases CD8 + T cell infiltration in vivo. Combined METTL5 targeting using lipid nanoparticle‐encapsulated siRNA and PD‐1 blockade provokes anti‐tumor immunity to eradicate ICC tumors. Additionally, METTL5 Low human ICC correlates with responsiveness to immunotherapy. The study highlights the strong immuno‐evasive ability of METTL5 as a promising therapeutic target in ICC.
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