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组成性地自发产生白细胞介素-1α或在白细胞介素-1α基因转移后产生白细胞介素-1α的纤维肉瘤的致瘤性降低。

Reduced tumorigenicity of fibrosarcomas which constitutively generate IL-1 alpha either spontaneously or following IL-1 alpha gene transfer.

作者信息

Douvdevani A, Huleihel M, Zöller M, Segal S, Apte R N

机构信息

Department of Microbiology and Immunology, Faculty of Health Sciences, Ben-Gurion University of The Negev, Beer-Sheva, Israel.

出版信息

Int J Cancer. 1992 Jul 9;51(5):822-30. doi: 10.1002/ijc.2910510526.

Abstract

Interleukin-1 (IL-1) is a major immunoregulatory/proinflammatory cytokine which also affects fibroblast proliferation and function and therefore it was of interest to investigate whether its constitutive expression influences the in vivo tumorigenic potential of transformed fibroblastoid cell lines. Here we report on a strong correlation between the constitutive expression of IL-1 alpha and reduced tumorigenicity, using various series of oncogene-transformed NIH/3T3-derived cell lines which produce the cytokine spontaneously or upon gene transfer, following transfection with the IL-1 alpha cDNA. Reduced tumorigenicity of the constitutive IL-1 alpha producing cell lines was manifested either by inability to grow in animals or by regressions of initially growing tumors, within 2 to 3 weeks from cell inoculation. In contrast, mice inoculated with non-IL-1-producing cell lines developed progressive tumors which ultimately killed the animals. Clones obtained from a non-IL-1-producing met-transformed cell line shifted from a progressive to a regressive phenotype, following transfection with an IL-1 alpha-encoding gene, inserted into an appropriate expression vector, resulting in constitutive expression of the cytokine. The effects of constitutive IL-1 expression on tumor development were observed both in histocompatible (NFS/N) and partially allogeneic (BALB/c) mice; however, they were more pronounced in the allogeneic environment. Fibrosarcomas which are non-IL-1 producers induced progressive tumors in both strains of mice at the same growth rate. The differences between the growth characteristics of the fibrosarcomas in histocompatible vs. partially allogenic mice suggest that IL-1 exerts adjuvant-like effects which increase the immunogenicity of tumor-cell antigens, and they also argue against the possibility that an IL-1-mediated local non-specific inflammatory response is the major effector mechanism of tumor rejection. Indeed, in subsequent studies we shall report on the importance of specific cellular immune responses, especially cytotoxic T lymphocytes (CTLs), in the eradication of constitutive IL-1-producing fibrosarcomas. Thus, our findings may serve as the basis for novel immunotherapy strategies aimed at the induction of IL-1 expression by cells comprising the neoplasm or alternatively by local application of the cytokine in the vicinity of the tumor.

摘要

白细胞介素-1(IL-1)是一种主要的免疫调节/促炎细胞因子,它也会影响成纤维细胞的增殖和功能,因此研究其组成性表达是否会影响转化的成纤维细胞样细胞系的体内致瘤潜力具有重要意义。在此,我们利用一系列经癌基因转化的源自NIH/3T3的细胞系进行报告,这些细胞系在转染IL-1α cDNA后,会自发产生细胞因子或经基因转移后产生细胞因子。我们发现IL-1α的组成性表达与致瘤性降低之间存在强烈的相关性。组成性产生IL-1α的细胞系致瘤性降低表现为无法在动物体内生长,或者在细胞接种后2至3周内,最初生长的肿瘤出现消退。相比之下,接种非产生IL-1细胞系的小鼠会形成进行性肿瘤,最终导致动物死亡。从一个非产生IL-1的met转化细胞系获得的克隆,在转染插入适当表达载体的编码IL-1α的基因后,从进行性表型转变为消退性表型,导致细胞因子的组成性表达。在组织相容性(NFS/N)和部分同种异体(BALB/c)小鼠中均观察到IL-1组成性表达对肿瘤发展的影响;然而,在同种异体环境中这种影响更为明显。非产生IL-1的纤维肉瘤在两种小鼠品系中均以相同的生长速率诱导进行性肿瘤。组织相容性小鼠与部分同种异体小鼠中纤维肉瘤生长特征的差异表明,IL-1发挥类似佐剂的作用,增加肿瘤细胞抗原的免疫原性,同时也排除了IL-1介导的局部非特异性炎症反应是肿瘤排斥主要效应机制的可能性。事实上,在后续研究中,我们将报告特异性细胞免疫反应,特别是细胞毒性T淋巴细胞(CTLs)在根除组成性产生IL-1的纤维肉瘤中的重要性。因此,我们的发现可能为新型免疫治疗策略提供基础,这些策略旨在诱导肿瘤组成细胞表达IL-1,或者在肿瘤附近局部应用细胞因子。

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