首页> 美国卫生研究院文献>Immunology >Interleukin-12 induces cytotoxic NK1+ alpha beta T cells in the lungs of euthymic and athymic mice.
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Interleukin-12 induces cytotoxic NK1+ alpha beta T cells in the lungs of euthymic and athymic mice.

机译:白细胞介素12诱导正常小鼠和无胸腺小鼠肺中的细胞毒性NK1 +αβT细胞。

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摘要

We recently reported that interleukin-12 (IL-12) stimulated hepatic NK1.1 Ag+ alpha beta T cells with intermediate T-cell receptor (TCR; NK1+ TCRint cells) and enhanced their NK1 expression (NK1high TCRint), and that these cells acquire strong major histocompatibility complex (MHC) unrestricted cytotoxicity in C57BL/6 mice, both +/+ and nu/nu. In the present study, we find that although murine lung normally has few NK1+ TCRint cells, NK1high TCRint cells are induced in+/+ and nu/nu mice after systemic administration of IL-12; these cells exhibit strong MHC unrestricted cytotoxicity against NK-sensitive and -resistant targets. A small number of NK1high TCRint cells was also found in peripheral blood after increased amounts of IL-12 were administered. Cytotoxicity tests in vitro revealed that the cytotoxic activity of the lung mononuclear cells (MNC) of C57BL/6 mice induced by IL-12 was abrogated by the depletion of either NK1+ or CD3+ cells, but not of CD8+ cells, as reportedly was the case of hepatic MNC, suggesting that NK1high TCRint cells are an antimetastatic population not only in the liver but also in the lung of mice. IL-12 injection into mice markedly elevates serum interferon-gamma (IFN-gamma) levels. However, although IL-12-induced cytotoxicity of NK1high TCRint cells was significantly reduced by anti-IFN-gamma antibody injection (which decreased serum IFN-gamma to an undetectable level), the appearance of NK1high TCRint cells in the lung and liver was not so affected. These results suggest that IFN-gamma is an important mediator of the cytotoxicity of NK1high TCRint cells but is not an essential factor for induction of these cells. We also added data showing that IL-12 has a broad antimetastatic effect against various liver and lung metastatic tumours intravenously injected into several strains of mice, including NK-deficient bg/bg mice. It can be considered that, in addition to NK cells, CD8+ cytotoxic T cells and gamma delta T cells, NK1+ TCRint cells can be categorized as one of the cytotoxic effector populations. These novel type cells distinct from regular T cells may play an important role in monitoring intra- and perivascular areas.
机译:我们最近报道说,白介素12(IL-12)刺激具有中间T细胞受体(TCR; NK1 + TCRint细胞)的肝NK1.1 Ag +αβT细胞并增强其NK1表达(NK1high TCRint),并且这些细胞获得了在C57BL / 6小鼠中,强的主要组织相容性复合物(MHC)不受限制的细胞毒性,包括+ / +和nu / nu。在本研究中,我们发现,尽管小鼠肺通常只有很少的NK1 + TCRint细胞,但是在全身性给予IL-12后,+ / +和nu / nu小鼠中都诱导了NK1high TCRint细胞。这些细胞对NK敏感和耐药的靶标表现出强大的MHC无限制的细胞毒性。给予高剂量的IL-12后,在外周血中也发现了少量的NK1high TCRint细胞。体外细胞毒性测试表明,IL-12诱导的C57BL / 6小鼠的肺单核细胞(MNC)的细胞毒性活性被NK1 +或CD3 +细胞的耗竭所废除,而CD8 +细胞的耗竭被废除了,据报道是这种情况肝MNC的研究表明NK1high TCRint细胞不仅在小鼠的肝脏中而且在小鼠的肺中都是一种抗转移人群。向小鼠注射IL-12可以显着提高血清干扰素-γ(IFN-γ)的水平。然而,尽管通过注射抗IFN-γ抗体显着降低了IL-12诱导的NK1high TCRint细胞的细胞毒性(将血清IFN-γ降低至无法检测的水平),但并未在肺和肝中出现NK1high TCRint细胞的出现。如此受影响。这些结果表明,IFN-γ是NK1high TCRint细胞的细胞毒性的重要介体,但不是诱导这些细胞的必要因素。我们还添加了数据,显示IL-12对静脉注射入几只小鼠模型(包括NK缺陷型bg / bg小鼠)的各种肝脏和肺部转移性肿瘤具有广泛的抗转移作用。可以认为,除了NK细胞,CD8 +细胞毒性T细胞和γ-δT细胞以外,NK1 + TCRint细胞也可以归类为细胞毒性效应物群体之一。这些不同于常规T细胞的新型细胞可能在监测血管内和血管周区域中起重要作用。

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