Hepatic regulatory T-cells promote colorectal liver metastasis in NASH

Jiannan Hu, Han Wang, Hongji Zhang, Jinghua Ren, Xiang Cheng, Yonghong Yao, A. Tsung, Hai Huang
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Abstract

Non-alcoholic steatohepatitis (NASH), a progressive inflammatory form of NAFLD, underlies an extremely versatile and dynamic inflammatory microenvironment along with aberrant metabolism and ongoing liver regeneration. Regulatory T cells (Tregs), as essential immune regulatory cells, are critical for the inhibition of tumor-promoting inflammation and cancer cell escape. Our recent study found that Tregs were selectively increased in both mouse models and patients with NAFLD, which promotes us to study the role of Tregs in NASH-HCC. However, the role of Tregs in the development of hepatic metastasis in NASH liver remains unknown. A Western diet mouse model and the STAM mouse model were utilized for NASH development. MC38 murine colorectal tumor cells were injected via portal vein at 12 weeks of feeding or orthotopically injected into cecum subserosa. Tumor development will be determined 3 or 4 weeks after injection. Depletion of Tregs by FoxP3-DTR mice or CD25 antibody treatment. Transcriptomic profiling of leucocytes in hepatic immune microenvironment was determined by scRNA-seq. There is a positive correlation between increased Tregs and hepatic tumor growth in NASH liver. Depleting Tregs inhibits the development of hepatic metastasis in NASH liver compared with control liver. NASH development led to a significant transcriptomic shift in hepatic immune cells, such as Kupffer cells, Tregs and MDSCs. Blocking the interaction of Tregs and PMN-MDSCs in the TME prevents tumor growth in the NASH liver. Tregs can suppress immunosurveillance in the premalignant stages of NASH. Therapies targeting Tregs could offer a potential strategy for preventing hepatic metastasis in patients with NASH. RO1GM137203
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肝调节性t细胞促进NASH患者结肠肝转移
非酒精性脂肪性肝炎(NASH)是NAFLD的一种进行性炎症形式,伴随异常代谢和持续的肝脏再生,形成了一个极其多样和动态的炎症微环境。调节性T细胞(Regulatory T cells, Tregs)作为重要的免疫调节细胞,在抑制促肿瘤炎症和癌细胞逃逸中起着至关重要的作用。我们最近的研究发现,在小鼠模型和NAFLD患者中,Tregs都有选择性地增加,这促使我们研究Tregs在NASH-HCC中的作用。然而,Tregs在NASH肝转移发展中的作用尚不清楚。采用西方饮食小鼠模型和STAM小鼠模型进行NASH发展。MC38小鼠结直肠肿瘤细胞于喂养12周时经门静脉注射或原位注射于盲肠浆膜下。注射后3 - 4周确定肿瘤的发展情况。FoxP3-DTR小鼠或CD25抗体处理对Tregs的消耗。采用scRNA-seq技术检测肝脏免疫微环境中白细胞的转录组学特征。在NASH肝中,Tregs升高与肝肿瘤生长呈正相关。与对照组相比,消耗Tregs抑制NASH肝转移的发展。NASH的发展导致肝免疫细胞(如Kupffer细胞、treg细胞和MDSCs)显著的转录组改变。阻断TME中Tregs和PMN-MDSCs的相互作用可阻止NASH肝脏中的肿瘤生长。Tregs可以抑制NASH恶性前期的免疫监视。针对Tregs的治疗可能为预防NASH患者肝转移提供一种潜在的策略。RO1GM137203
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