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本文引用的文献

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Nicotine Upregulates the Level of Mcl-1 through STAT3 in H1299 Cells.尼古丁通过信号转导和转录激活因子3(STAT3)上调H1299细胞中髓细胞白血病序列1(Mcl-1)的水平。
J Cancer. 2020 Jan 1;11(5):1270-1276. doi: 10.7150/jca.35453. eCollection 2020.
2
PD1 CD8 T cells correlate with exhausted signature and poor clinical outcome in hepatocellular carcinoma.PD1 CD8 T 细胞与肝癌衰竭特征和不良临床结局相关。
J Immunother Cancer. 2019 Nov 29;7(1):331. doi: 10.1186/s40425-019-0814-7.
3
STAT3 Activation-Induced Fatty Acid Oxidation in CD8 T Effector Cells Is Critical for Obesity-Promoted Breast Tumor Growth.信号转导和转录激活因子3(STAT3)激活诱导的CD8效应T细胞脂肪酸氧化对肥胖促进的乳腺肿瘤生长至关重要。
Cell Metab. 2020 Jan 7;31(1):148-161.e5. doi: 10.1016/j.cmet.2019.10.013. Epub 2019 Nov 21.
4
Cholesterol Induces CD8 T Cell Exhaustion in the Tumor Microenvironment.胆固醇在肿瘤微环境中诱导 CD8 T 细胞耗竭。
Cell Metab. 2019 Jul 2;30(1):143-156.e5. doi: 10.1016/j.cmet.2019.04.002. Epub 2019 Apr 25.
5
Low and variable tumor reactivity of the intratumoral TCR repertoire in human cancers.人类肿瘤中肿瘤内 TCR 库的低反应性和变异性。
Nat Med. 2019 Jan;25(1):89-94. doi: 10.1038/s41591-018-0266-5. Epub 2018 Dec 3.
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Targeting colon cancer with the novel STAT3 inhibitor bruceantinol.用新型 STAT3 抑制剂布鲁斯替尼靶向治疗结肠癌。
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The Effectiveness of Checkpoint Inhibitor Combinations and Administration Timing Can Be Measured by Granzyme B PET Imaging.基于颗粒酶 B PET 成像技术,可评估检查点抑制剂联合治疗的有效性和用药时机。
Clin Cancer Res. 2019 Feb 15;25(4):1196-1205. doi: 10.1158/1078-0432.CCR-18-2407. Epub 2018 Oct 16.
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Improving the Efficiency of Vγ9Vδ2 T-Cell Immunotherapy in Cancer.提高 Vγ9Vδ2 T 细胞免疫疗法在癌症治疗中的效率。
Front Immunol. 2018 Apr 19;9:800. doi: 10.3389/fimmu.2018.00800. eCollection 2018.
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Regulatory T cells: a potential target in cancer immunotherapy.调节性 T 细胞:癌症免疫治疗的一个潜在靶点。
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10
Transcription Factor IRF4 Promotes CD8 T Cell Exhaustion and Limits the Development of Memory-like T Cells during Chronic Infection.转录因子 IRF4 促进慢性感染期间 CD8 T 细胞耗竭并限制记忆样 T 细胞的发育。
Immunity. 2017 Dec 19;47(6):1129-1141.e5. doi: 10.1016/j.immuni.2017.11.021. Epub 2017 Dec 12.

尼古丁通过增加 miR-629-5p 抑制 IL2RB 介导的颗粒酶 B 表达来耗尽 CD8 T 细胞对肿瘤细胞的作用。

Nicotine exhausts CD8 T cells against tumor cells through increasing miR-629-5p to repress IL2RB-mediated granzyme B expression.

机构信息

Radiation Biology Research Center, Institute for Radiological Research, Chang Gung Memorial Hospital, Chang Gung University, Linkou, Taiwan.

Division of Gastroenterology, Cheng Hsin General Hospital, Taipei, Taiwan.

出版信息

Cancer Immunol Immunother. 2021 May;70(5):1351-1364. doi: 10.1007/s00262-020-02770-x. Epub 2020 Nov 3.

DOI:10.1007/s00262-020-02770-x
PMID:33146402
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10991426/
Abstract

The mechanism exhausting CD8 T cells is not completely clear against tumors. Literature has demonstrated that cigarette smoking disables the immunological activity, so we propose nicotine is able to exhaust CD8 T cells. The CD8 T cells from healthy volunteers with and without cigarette smoking and the capacity of CD8 T cells against tumor cells were investigated. RNAseq was used to investigate the gene profiling expression in CD8 T cells. Meanwhile, small RNAseq was also used to search novel microRNAs involved in the exhaustion of CD8 T cells. The effect of nicotine exhausting CD8 T cells was investigated in vitro and in the humanized tumor xenografts in vivo. We found that CD8 T cells were able to reduce cell viability in lung cancer HCC827 and A549 cells, that secreted granzyme B, but CD8 T cells from the healthy cigarette smokers lost anti-HCC827 effect. Moreover, nicotine suppressed the anti-HCC827 effect of CD8 T cells. RNAseq revealed lower levels of IL2RB and GZMB in the exhausted CD8 T cells. We identified that miR-629-5p was increased by nicotine, that targeted IL2RB. Transfection of miR-629-5p mimic reduced IL2RB and GZMB levels. We further validated that nicotine reduced granzyme B levels using a nuclear imaging technique, and demonstrated that nicotine exhausted peripheral blood mononuclear cells against HCC827 growth in the humanized tumor xenografts. This study demonstrated that nicotine exhausted CD8 T cells against HCC827 cells through increasing miR-629-5p to suppress IL2RB.

摘要

针对肿瘤,耗竭 CD8 T 细胞的机制尚不完全清楚。文献表明,吸烟会使免疫活性丧失,因此我们提出尼古丁能够耗竭 CD8 T 细胞。本研究旨在调查健康志愿者中有无吸烟史的 CD8 T 细胞及其对肿瘤细胞的活性,并通过 RNAseq 研究 CD8 T 细胞中的基因表达谱,同时通过小 RNAseq 寻找参与 CD8 T 细胞耗竭的新型 microRNA。我们在体外和人源化肿瘤异种移植模型中研究了尼古丁对 CD8 T 细胞的耗竭作用。我们发现 CD8 T 细胞能够降低肺癌 HCC827 和 A549 细胞的活力并分泌颗粒酶 B,但来自健康吸烟者的 CD8 T 细胞丧失了抗 HCC827 作用。此外,尼古丁抑制了 CD8 T 细胞的抗 HCC827 作用。RNAseq 显示耗竭的 CD8 T 细胞中 IL2RB 和 GZMB 的水平降低。我们发现尼古丁增加了靶向 IL2RB 的 microRNA-629-5p,转染 miR-629-5p 模拟物可降低 IL2RB 和 GZMB 水平。我们进一步使用核成像技术验证了尼古丁降低了颗粒酶 B 水平,并证明尼古丁通过增加 miR-629-5p 来抑制 IL2RB,从而耗竭外周血单核细胞对 HCC827 生长的抑制作用。本研究表明,尼古丁通过增加 miR-629-5p 抑制 IL2RB 来耗竭 CD8 T 细胞,从而抑制 HCC827 细胞。