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癌基因转化的纤维肉瘤细胞系中白细胞介素-1表达的异常:白细胞介素-1α的组成型转录及生物活性表现

Aberrations in interleukin-1 expression in oncogene-transformed fibrosarcoma lines: constitutive interleukin-1 alpha transcription and manifestation of biological activity.

作者信息

Douvdevani A, Huleihel 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

Eur Cytokine Netw. 1991 Aug-Sep;2(4):257-64.

PMID:1756231
Abstract

We have examined interleukin-1 (IL-1) expression in a series of oncogene-transformed NIH-3T3 fibroblastoid cell lines. In contrast to primary fibroblasts where IL-1 is inducible, NIH-3T3 cells (clone 490N3T) transcribe the IL-1 alpha gene constitutively. Transformation of 490N3T cells by the v-mos or v-H-ras oncogenes appears to either enhance or suppress IL-1 alpha transcription, respectively. In v-myc transfected cells, constitutive IL-1 activity could be detected intracellularly. An additional membrane-associated form of IL-1 was observed in lines transformed by protein-kinase (PK) encoding oncogenes, such as TPR-met, c-met, v-src, v-abl, v-mos and v-raf. In none of the lines tested the secreted form of IL-1 activity could be detected, and no constitutive expression of IL-1 beta was observed. Our studies manifest aberrations in IL-1 expression in oncogene-transformed fibroblastoid cell lines, detected at different regulatory levels, such as transcription, translation and compartmentalization. IL-1 is a potent pleiotropic cytokine, with regard to its target cell specificity and spectrum of activities; growth promoting effects of IL-1 on fibroblasts were reported and on the other hand this cytokine activates various anti-tumor mechanisms. Thus, endogenous IL-1 expression by tumor cells may affect the neoplastic phenotype, either by influencing the growth of the malignant cells or by modifying tumor-host interactions.

摘要

我们检测了一系列癌基因转化的NIH-3T3成纤维细胞样细胞系中白细胞介素-1(IL-1)的表达情况。与可诱导IL-1表达的原代成纤维细胞不同,NIH-3T3细胞(克隆490N3T)组成性转录IL-1α基因。v-mos或v-H-ras癌基因对490N3T细胞的转化似乎分别增强或抑制了IL-1α的转录。在v-myc转染的细胞中,可在细胞内检测到组成性的IL-1活性。在由编码蛋白激酶(PK)的癌基因(如TPR-met、c-met、v-src、v-abl、v-mos和v-raf)转化的细胞系中,观察到了另一种与膜相关的IL-1形式。在所检测的细胞系中,均未检测到IL-1活性的分泌形式,也未观察到IL-1β的组成性表达。我们的研究表明,在癌基因转化的成纤维细胞样细胞系中,IL-1表达存在异常,这种异常在转录、翻译和区室化等不同调控水平上均可检测到。IL-1是一种强效的多效性细胞因子,就其靶细胞特异性和活性谱而言;有报道称IL-1对成纤维细胞有促生长作用,另一方面,这种细胞因子还可激活多种抗肿瘤机制。因此,肿瘤细胞内源性IL-1的表达可能会影响肿瘤表型,要么通过影响恶性细胞的生长,要么通过改变肿瘤与宿主的相互作用来实现。

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