IRE1信号的抑制影响编码tnf相关因子和受体的亚基因的表达,并改变其在U87胶质瘤细胞中的缺氧调节

IF 0.7
O. Minchenko, I. V. Kryvdiuk, D. Minchenko, O. O. Riabovol, O. V. Halkin
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引用次数: 10

摘要

IRE1(肌醇要求酶-1)是内质网应激的主要信号通路,抑制IRE1可显著降低胶质瘤细胞的生长和增殖。为了阐明IRE1介导胶质瘤生长的作用,我们研究了编码TNF(肿瘤坏死因子)相关因子和受体的亚基因在过表达显性负IRE1 (dnIRE1)的U87胶质瘤细胞中的表达及其缺氧调节。我们发现,在IRE1修饰的胶质瘤细胞中,TNFAIP1、TNFRSF10D、TNFRSF21、TNFRSF11B、TNFSF7和LITAF基因的表达增加;然而,与对照细胞相比,TNFRSF10B、TRADD和TNFAIP3在这些细胞中下调。在这个实验条件下,我们没有发现TNFRSF1A基因表达有明显变化。在对照胶质瘤细胞中,缺氧导致TNFAIP1、TNFAIP3、TRADD和TNFRSF10D基因表达上调,同时TNFRSF21、TNFRSF11B和LITAF基因表达下调;而TNFRSF10B和TNFRSF1A基因对缺氧处理具有抗性。然而,IRE1的抑制改变了LITAF、TNFRSF21、TNFRSF11B和TRADD基因的缺氧调控,并引入了缺氧诱导的对TNFRSF10B、TNFRSF1A和TNFSF7基因表达的敏感性。此外,通过siRNA敲低tnfrsf21mrna可以改变缺氧对U87胶质瘤细胞ire1依赖性增殖率和细胞死亡的影响。目前的研究表明,与细胞死亡和增殖直接相关的tnf相关因子和受体的表达的微调操纵是由内质网应激效应物IRE1以及缺氧以基因特异性的方式介导的。因此,IRE1激酶和核糖核酸内切酶活性的抑制与tnf相关因子和受体的解除相关,这种方式是基因特异性的,从而减缓肿瘤生长。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Inhibition of IRE1 signaling affects expression of a subset genes encoding for TNF-related factors and receptors and modifies their hypoxic regulation in U87 glioma cells
Abstract Inhibition of IRE1 (inositol requiring enzyme-1), the major signaling pathway of endoplasmic reticulum stress, significantly decreases tumor growth and proliferation of glioma cells. To elucidate the role of IRE1- mediated glioma growth, we studied the expression of a subset genes encoding for TNF (tumor necrosis factor)- related factors and receptors and their hypoxic regulation in U87 glioma cells overexpressing dominant-negative IRE1 (dnIRE1). We demonstrated that the expression of TNFAIP1, TNFRSF10D, TNFRSF21, TNFRSF11B, TNFSF7, and LITAF genes is increased in glioma cells with modified IRE1; however, TNFRSF10B, TRADD, and TNFAIP3 is down-regulated in these cells as compared to their control counterparts. We did not find TNFRSF1A gene expression to change significantly under this experimental condition. In control glioma cells, hypoxia leads to the up-regulated expression of TNFAIP1, TNFAIP3, TRADD, and TNFRSF10D genes and the concomitant down-regulation of TNFRSF21, TNFRSF11B, and LITAF genes; while, TNFRSF10B and TNFRSF1A genes are resistant to hypoxic treatment. However, inhibition of IRE1 modifies the hypoxic regulation of LITAF, TNFRSF21, TNFRSF11B, and TRADD genes and introduces hypoxia-induced sensitivity to TNFRSF10B, TNFRSF1A, and TNFSF7 gene expressions. Furthermore, knockdown by siRNA of TNFRSF21 mRNA modifies the hypoxic effect on the IRE1-dependent rate of proliferation and cell death in U87 glioma cells. The present study demonstrates that fine-tuned manipulation of the expression of TNF-related factors and receptors directly relating to cell death and proliferation, is mediated by an effector of endoplasmic reticulum stress, IRE1, as well as by hypoxia in a gene-specific manner. Thus, inhibition of the kinase and endoribonuclease activities of IRE1 correlates with deregulation of TNF-related factors and receptors in a manner that is gene specific and thus slows tumor growth.
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