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NK Cells Stimulate Recruitment of cDC1 into the Tumor Microenvironment Promoting Cancer Immune Control

机译:NK细胞刺激CDC1募集到肿瘤微环境促进癌症免疫控制

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摘要

Conventional type 1 dendritic cells (cDC1) are critical for antitumor immunity, and their abundance within tumors is associated with immune-mediated rejection and the success of immunotherapy. Here, we show that cDC1 accumulation in mouse tumors often depends on natural killer (NK) cells that produce the cDC1 chemoattractants CCL5 and XCL1. Similarly, in human cancers, intratumoral CCL5, XCL1, and XCL2 transcripts closely correlate with gene signatures of both NK cells and cDC1 and are associated with increased overall patient survival. Notably, tumor production of prostaglandin E2 (PGE(2)) leads to evasion of the NK cell-cDC1 axis in part by impairing NK cell viability and chemokine production, as well as by causing downregulation of chemokine receptor expression in cDC1. Our findings reveal a cellular and molecular checkpoint for intratumoral cDC1 recruitment that is targeted by tumor-derived PGE(2) for immune evasion and that could be exploited for cancer therapy.
机译:常规1型树突细胞(CDC1)对于抗肿瘤免疫力至关重要,并且它们在肿瘤内的丰度与免疫介导的排斥和免疫疗法的成功有关。 在这里,我们表明,小鼠肿瘤中的CDC1积累往往取决于产生CCL5和XCl1的CCL5和XCl1的天然杀伤(NK)细胞。 类似地,在人类癌症中,腹腔内CCl5,XCl1和XCl2转录物与NK细胞和CDC1的基因特征密切相关,并且与增加的整体患者存活率相关。 值得注意的是,通过损害NK细胞活力和趋化因子的产生,以及通过导致CDC1中的趋化因子受体表达的下调,前列腺素E2(PGE(2))的肿瘤产生导致NK细胞-CDC1轴的疏散,以及趋化因子的下调。 我们的研究结果揭示了肿瘤内CDC1募集的细胞和分子检查点,其是由肿瘤衍生的PGE(2)靶向的免疫逃避,可用于癌症治疗。

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  • 来源
    《Cell》 |2018年第5期|共30页
  • 作者单位

    Francis Crick Inst Immunobiol Lab 1 Midland Rd London NW1 1AT England;

    Univ Manchester CRUK Manchester Inst Canc Inflammat &

    Immun Grp Manchester M20 4BX Lancs England;

    Francis Crick Inst Bioinformat 1 Midland Rd London NW1 1AT England;

    Francis Crick Inst Immunobiol Lab 1 Midland Rd London NW1 1AT England;

    Francis Crick Inst Immunobiol Lab 1 Midland Rd London NW1 1AT England;

    Francis Crick Inst Immunobiol Lab 1 Midland Rd London NW1 1AT England;

    Francis Crick Inst Immunobiol Lab 1 Midland Rd London NW1 1AT England;

    Francis Crick Inst Tumour Cell Biol Lab 1 Midland Rd London NW1 1AT England;

    Univ Manchester CRUK Manchester Inst Canc Inflammat &

    Immun Grp Manchester M20 4BX Lancs England;

    Francis Crick Inst Immunobiol Lab 1 Midland Rd London NW1 1AT England;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 细胞生物学;
  • 关键词

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