Expression of proliferation related transcription factor genes in U87 glioma cells with IRE1 knockdown: upon glucose and glutamine deprivation.

D O Tsymbal, D O Minchenko, I V Kryvdiuk, O O Riabovo, O O Halkin, O O Ratushna, O H Minchenko
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引用次数: 13

Abstract

Glycolysis and glutaminolysis as well as endoplasmic reticulum stress are required for tumor progression suggests through regulation of the cell cycle. Inhibition of ERN1/IRE1 (endoplasmic reticulum to nucleus signaling 1/inositol requiring enzyme 1), a central mediator of endoplasmic reticulum stress, significantly suppresses glioma cell proliferation and tumor growth as well as modifies sensitivity gene expressions to glucose and glutamine deprivation. We have studied the expression of genes encoded transcription factors such as E2F8 (E2F transcription factor 8), EPAS1 (endothelial PAS domain protein 1), HOXC6 (homeobox C6), TBX3 (T-box 3), TBX2 (T-box 2), GTF2F2 (general transcription factor IIF), GTF2B (general transcription factor IIB), MAZ (MYC-associated zinc finger protein, purine-binding transcription factor), SNAI2 (snail family zinc finger 2), TCF3 (transcription factor 3), and TCF8/ZEB1 (zinc finger E-box binding homeobox 1)in U87 glioma cells upon glucose and glutamine deprivation in relation to inhibition of IRE1.We demonstrated that glutamine deprivation leads to up-regulation of the expression of EPAS1, TBX3, GTF2B, and MAZ genes and down-regulation of E2F8, GTF2F2, TCF8, and TBX2 genes in control glioma cells.At the same time, glucose deprivation enhances the expression of EPAS1 and GTF2B genes and decreases of E2F8, HOXC6, TCF3, and TBX2 genes in these glioma cells. Inhibition of IRE1 by dnIRE1 significantly modifies the expression most of studied genes with different magnitude. Present study demonstrates that fine-tuning of the expression of proliferation related transcription factor genes depends upon glucose and glutamine deprivation in IRE1-dependent manner and possibly contributes to slower tumor growth after inhibition of IRE1.

葡萄糖和谷氨酰胺剥夺后IRE1基因敲低的U87胶质瘤细胞中增殖相关转录因子基因的表达
糖酵解和谷氨酰胺解以及内质网应激是肿瘤进展所必需的,这表明通过调节细胞周期。ERN1/IRE1(内质网对核信号传导1/肌醇要求酶1)是内质网应激的中心介质,抑制ERN1/IRE1可显著抑制胶质瘤细胞增殖和肿瘤生长,并改变对葡萄糖和谷氨酰胺剥夺的敏感性基因表达。我们研究了E2F8 (E2F转录因子8)、EPAS1(内皮PAS结构域蛋白1)、HOXC6(同源盒C6)、TBX3 (T-box 3)、TBX2 (T-box 2)、GTF2F2(一般转录因子IIF)、GTF2B(一般转录因子IIB)、MAZ (myc相关锌指蛋白、嘌呤结合转录因子)、SNAI2(蜗牛家族锌指2)、TCF3(转录因子3)、葡萄糖和谷氨酰胺剥夺后U87胶质瘤细胞中TCF8/ZEB1(锌指E-box binding homeobox 1)与IRE1抑制的关系。我们发现,在对照胶质瘤细胞中,谷氨酰胺剥夺导致EPAS1、TBX3、GTF2B和MAZ基因表达上调,E2F8、GTF2F2、TCF8和TBX2基因表达下调。同时,葡萄糖剥夺可增强这些胶质瘤细胞中EPAS1和GTF2B基因的表达,降低E2F8、HOXC6、TCF3和TBX2基因的表达。dnIRE1对IRE1的抑制作用对大部分研究基因的表达有不同程度的显著改变。目前的研究表明,增殖相关转录因子基因的表达微调依赖于IRE1依赖性的葡萄糖和谷氨酰胺剥夺,可能有助于抑制IRE1后肿瘤生长减慢。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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