Department of Surgery, Kaohsiung Veterans General Hospital Tainan Branch, Tainan, Taiwan.
Institute of Clinical Medicine, College of Medicine, National Cheng Kung University, Tainan, Taiwan.
Cancer Immunol Immunother. 2024 Jan 4;73(1):1. doi: 10.1007/s00262-023-03601-5.
Tumor-associated macrophages (TAMs) are the predominant immune cells in the tumor microenvironment and portend poor prognosis. However, the molecular mechanisms underlying the tumor promotion of TAMs have not been fully elucidated.
Coculture of gastric cancer cells with U937 cells was performed to investigate the impact of TAMs on cancer cell behavior. MicroRNA (miRNA) microarray and bioinformatics were applied to identify the involved miRNAs and the functional target genes. The regulation of the miRNA on its target gene was studied using anti-miRNA and miRNA mimic.
Coculture with CD204 M2-like TAMs increased proliferation, migration, and epithelial-mesenchymal transition of gastric cancer cells. MiR-210 was the most upregulated miRNA in cancer cells identified by miRNA microarray after coculture. In gastric cancer tissues, miR-210 expression was positively correlated with CD204 M2-like TAM infiltration. Inactivation of miR-210 by antimir attenuated CD204 M2-like TAMs-induced cancer cell migration. Using pharmacological inhibitors and neutralizing antibodies, CD204 M2-like TAMs-secreted TNFα was found to upregulate miR-210 through NF-κB/HIF-1α signaling. Bioinformatics analysis showed netrin-4 (NTN4) as a potential target of miR-210 to suppress gastric cancer cell migration. We also found an inverse expression between miR-210 and NTN4 in cancer cells after coculture or in tumor xenografts. Anti-miR-210 increased NTN4 expression, while miR-210 mimics downregulated NTN4 in cancer cells. Reporter luciferase assays showed that MiR-210 mimics suppressed NTN4 3' untranslated region-driven luciferase activity in cancer cells, but this effect was blocked after mutating miR-210 binding site.
CD204 M2-like TAMs can utilize the TNF-α/NF-κB/HIF-1α/miR-210/NTN4 pathway to facilitate gastric cancer progression.
肿瘤相关巨噬细胞(TAMs)是肿瘤微环境中的主要免疫细胞,预示着预后不良。然而,TAMs 促进肿瘤的分子机制尚未完全阐明。
通过共培养胃癌细胞和 U937 细胞来研究 TAMs 对癌细胞行为的影响。应用 miRNA 微阵列和生物信息学来鉴定涉及的 miRNA 和功能靶基因。通过使用抗 miRNA 和 miRNA 模拟物来研究 miRNA 对其靶基因的调控。
与 CD204 M2 样 TAMs 共培养可增加胃癌细胞的增殖、迁移和上皮间质转化。miRNA 微阵列鉴定出共培养后癌细胞中上调最显著的 miRNA 是 miR-210。在胃癌组织中,miR-210 的表达与 CD204 M2 样 TAM 浸润呈正相关。用抗 miRNA 使 miR-210 失活可减弱 CD204 M2 样 TAMs 诱导的癌细胞迁移。使用药理学抑制剂和中和抗体发现,CD204 M2 样 TAMs 分泌的 TNFα 通过 NF-κB/HIF-1α 信号通路上调 miR-210。生物信息学分析显示,轴突导向因子 netrin-4(NTN4)是 miR-210 抑制胃癌细胞迁移的潜在靶标。我们还发现,共培养或肿瘤异种移植后癌细胞中 miR-210 和 NTN4 的表达呈负相关。抗 miR-210 增加了癌细胞中 NTN4 的表达,而 miR-210 模拟物则下调了癌细胞中的 NTN4。报告基因荧光素酶实验显示,miR-210 模拟物抑制了癌细胞中 NTN4 3'UTR 驱动的荧光素酶活性,但在突变 miR-210 结合位点后,这种作用被阻断。
CD204 M2 样 TAMs 可利用 TNF-α/NF-κB/HIF-1α/miR-210/NTN4 通路促进胃癌进展。
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