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白细胞介素-1 分子对 3-MCA 诱导细胞系生长模式的影响:免疫原性和侵袭潜能之间的相互作用。

Effects of IL-1 molecules on growth patterns of 3-MCA-induced cell lines: an interplay between immunogenicity and invasive potential.

机构信息

The Shraga Segal Department of Microbiology and Immunology, Faculty of Health Sciences and The Cancer Research Center, Ben-Gurion University of the Negev, Beer-Sheva, Israel.

出版信息

J Immunotoxicol. 2010 Mar;7(1):27-38. doi: 10.3109/15476910903405528.

Abstract

The balance between inflammation and immunity is cardinal for the outcome of the malignant process. Local attenuated inflammatory responses mediated by innate cells may provide accessory signals for the development of acquired immunity against malignant cells. In contrast, excessive inflammatory responses accompany tumorigenesis and tumor invasiveness, by the induction of immunosuppression. In the present study, we have assessed the role of tumor cell-derived IL-1 in determining the invasive versus immunostimulatory potential of tumor cells. For this purpose, we have used 3-MCA-induced fibrosarcoma cell lines from IL-1 knockout (KO) versus control mice. Cell lines with no IL-1 failed to establish tumors in intact mice, while lines obtained from control mice were invasive and induced a potent angiogenic response. In contrast, cell lines from IL-1KO mice were more immunogenic. SDF-1 and IL-6, each induced by IL-1, were the two major cytokines whose levels differed in cell lines with or without IL-1. We could not detect differences in cell surface markers related to immunogenicity, such as MHC Class I, co-stimulatory, or adhesion molecules between both types of cells. However, more T-cells were observed at the inoculation site of tumor cells devoid of IL-1 and more pronounced parameters related to anti-tumor immunity were observed in the spleen (IL-12 and IFNgamma) of these mice, compared to mice bearing tumors derived from control mice, where host-derived IL-1 is present. In addition, injection of tumor cells devoid of IL-1, which failed to grow in mice, induced an anti-tumor cell immune memory, while in mice injected with tumor cells from control mice; no immune memory could be detected. From the results, it seems that IL-1 is a crucial factor in determining the balance between immunity and inflammation in tumor-bearing mice. This suggests that manipulation of IL-1 could be useful in anti-tumor therapy, by reducing invasiveness and promoting immunity against the malignant cells.

摘要

炎症与免疫之间的平衡对于恶性过程的结果至关重要。先天细胞介导的局部减弱的炎症反应可能为获得性免疫提供辅助信号,以对抗恶性细胞。相反,过度的炎症反应伴随着肿瘤发生和肿瘤侵袭,诱导免疫抑制。在本研究中,我们评估了肿瘤细胞衍生的 IL-1 在决定肿瘤细胞的侵袭性与免疫刺激性潜能之间的作用。为此,我们使用了来自 IL-1 敲除(KO)和对照小鼠的 3-MCA 诱导纤维肉瘤细胞系。没有 IL-1 的细胞系在完整的小鼠中无法建立肿瘤,而来自对照小鼠的细胞系具有侵袭性,并诱导强烈的血管生成反应。相比之下,来自 IL-1KO 小鼠的细胞系更具免疫原性。SDF-1 和 IL-6,每种都由 IL-1 诱导,是两种主要的细胞因子,其在具有或不具有 IL-1 的细胞系中的水平不同。我们无法检测到与免疫原性相关的细胞表面标志物(如 MHC 类 I、共刺激或粘附分子)在这两种类型的细胞之间存在差异。然而,在缺乏 IL-1 的肿瘤细胞接种部位观察到更多的 T 细胞,并且在这些小鼠的脾脏中观察到与抗肿瘤免疫相关的更明显的参数(IL-12 和 IFNgamma),与携带来自对照小鼠的肿瘤的小鼠相比,其中存在宿主衍生的 IL-1。此外,注射在小鼠中无法生长的缺乏 IL-1 的肿瘤细胞会诱导抗肿瘤细胞免疫记忆,而在注射来自对照小鼠的肿瘤细胞的小鼠中,则无法检测到免疫记忆。从结果来看,IL-1 似乎是决定荷瘤小鼠中免疫与炎症之间平衡的关键因素。这表明操纵 IL-1 可能有助于抗肿瘤治疗,通过减少侵袭性并促进对恶性细胞的免疫。

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