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

Tsymbal, Dariia O.; Minchenko, Dmytro O.; Kryvdiuk, Iryna V.; Riabovo, O O; Halkin, O O; Ratushna, O O; Minchenko, О. H.

doi:10.15407/fz62.01.003

Cited by 10 publications

(10 citation statements)

References 40 publications

(70 reference statements)

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“…Previously was shown that glutamine withdrawal affected the expression of several tumor growth related genes and that the effect of glutamine deprivation on most of these genes expression is dependent on ERN1 signaling enzyme function [19][20][21][22][23]. However, the regulation of the expression of many other tumor growth related genes by glutamine deprivation in relation to inhibition of ERN1 to not to be clarified yet.…”

Section: The Expression Of a Subset Of Genes Encoding Important Tumormentioning

confidence: 99%

ERN1 modifies the effect of glutamine deprivation on tumor growth related factors expression in U87 glioma cells

Minchenko¹,

Kharkova²,

Hnatiuk³

2018

Ukr.Biochem.J

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Section: The Expression Of a Subset Of Genes Encoding Important Tumormentioning

confidence: 99%

ERN1 modifies the effect of glutamine deprivation on tumor growth related factors expression in U87 glioma cells

Minchenko¹,

Kharkova²,

Hnatiuk³

2018

Ukr.Biochem.J

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“…Glutamine, as a substrate for glycolysis, is an important for the development and a more aggressive behavior of gliomas, which are highly aggressive tumors with very poor prognosis (Colombo et al 2011;Yalcin et al 2014;Zhao et al 2017;Alimohammadi et al 2020). Glutamine supply and endoplasmic reticulum stress are very important and complementary factors for the tumor growth and inhibition of ERN1/IRE1 (endoplasmic reticulum to nucleus signaling 1/inositol requiring enzyme 1) mediated stress signaling can significantly modify the effects of glutamine deprivation on some gene expressions (Minchenko et al 2013(Minchenko et al , 2015a(Minchenko et al , 2021Tsymbal et al 2016). It has been shown that ERN1 -XBP1 pathway is also essential for the glucose response and protection of β cells (Riabovol et al 2019).…”

mentioning

confidence: 99%

“…Transcription factors play an important role in malignant tumor growth preferentially through ERN1 (endoplasmic reticulum to nucleus signaling 1) signaling pathway of endoplasmic reticulum stress (Minchenko et al 2015b(Minchenko et al , 2015cTsymbal et al 2016). The homeobox proteins represent an important group of transcription factors, which are related to tumorigenesis and are largely investigated (Guca et al 2018;Le Magnen et al 2018;Miyashita et al 2018;Hamaidi et al 2019;Li et al 2019).…”

mentioning

confidence: 99%

The impact of glutamine deprivation on the expression of MEIS3, SPAG4, LHX1, LHX2, and LHX6 genes in ERN1 knockdown U87 glioma cells

Krasnytska

Khita

Tsymbal

et al. 2022

Endocrine Regulations

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Objective. The aim of the current study was to investigate the expression of genes encoded homeobox proteins such as MEIS3 (Meis homeobox 3), SPAG4 (sperm associated antigen 4), LHX1 (LIM homeobox 1), LHX2, and LHX6 in U87 glioma cells in response to glutamine deprivation in control glioma cells and cells with knockdown of ERN1 (endoplasmic reticulum to nucleus signaling 1), the major pathway of the endoplasmic reticulum stress signaling, for evaluation of a possible dependence on the expression of these important regulatory genes from glutamine supply and ERN1 signaling. Methods. The expression level of MEIS3, SPAG4, LHX, LHX2, and LHX6 genes was studied by real-time quantitative polymerase chain reaction in control U87 glioma cells (transfected by vector) and cells with ERN1 knockdown after exposure to glutamine deprivation. Results. It was shown that the expression level of MEIS3 and LHX1 genes was up-regulated in control glioma cells treated by glutamine deprivation. At the same time, the expression level of three other genes (LHX2, LHX6, and SPAG4) was down-regulated. Furthermore, ERN1 knockdown significantly modified the effect of glutamine deprivation on LHX1 gene expression in glioma cells, but did not change significantly the sensitivity of all other genes expression to this experimental condition. Conclusion. The results of this investigation demonstrate that the exposure of U87 glioma cells under glutamine deprivation significantly affected the expression of all genes studied encoding the homeobox proteins and that this effect of glutamine deprivation was independent of the endoplasmic reticulum stress signaling mediated by ERN1, except LHX1 gene.

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“…After WGCNA and protein–protein interaction (PPI) analysis, general transcription factor IIF polypeptide 2 ( GTF2F2 ) was identified as the hub gene. GTF2F2 combines with general transcription factor IIF polypeptide 1 (GTF2F1) to form a heteromeric general transcription initiation factor (TFIIF), which subsequently binds to DNA-dependent RNA polymerase II ( Sasaki et al, 2013 ; Tsymbal et al, 2016 ). RNA polymerase II plays a critical role in mRNA synthesis, and GTF2F2 is essential for the initiation and elongation phases of gene transcription ( Sasaki et al, 2013 ).…”

Section: Introductionmentioning

confidence: 99%

General Transcription Factor IIF Polypeptide 2: A Novel Therapeutic Target for Depression Identified Using an Integrated Bioinformatic Analysis

Zhang

Cheng

Dong

et al. 2022

Front. Aging Neurosci.

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Depression currently affects 4% of the world’s population; it is associated with disability in 11% of the global population. Moreover, there are limited resources to treat depression effectively. Therefore, we aimed to identify a promising novel therapeutic target for depression using bioinformatic analysis. The GSE54568, GSE54570, GSE87610, and GSE92538 gene expression data profiles were retrieved from the Gene Expression Omnibus (GEO) database. We prepared the four GEO profiles for differential analysis, protein–protein interaction (PPI) network construction, and weighted gene co-expression network analysis (WGCNA). Gene Ontology functional enrichment and Kyoto Encyclopedia of Genes and Genomes metabolic pathway analyses were conducted to determine the key functions of the corresponding genes. Additionally, we performed correlation analyses of the hub genes with transcription factors, immune genes, and N6-methyladenosine (m6A) genes to reveal the functional landscape of the core genes associated with depression. Compared with the control samples, the depression samples contained 110 differentially expressed genes (DEGs), which comprised 56 downregulated and 54 upregulated DEGs. Moreover, using the WGCNA and PPI clustering analysis, the blue module and cluster 1 were found to be significantly correlated with depression. GTF2F2 was the only common gene identified using the differential analysis and WGCNA; thus, it was used as the hub gene. According to the enrichment analyses, GTF2F2 was predominantly involved in the cell cycle and JAK-STAT, PI3K-Akt, and p53 signaling pathways. Furthermore, differential and correlation analyses revealed that 9 transcription factors, 12 immune genes, and 2 m6A genes were associated with GTF2F2 in depression samples. GTF2F2 may serve as a promising diagnostic biomarker and treatment target of depression, and this study provides a novel perspective and valuable information to explore the molecular mechanism of depression.

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

Cited by 10 publications

References 40 publications

ERN1 modifies the effect of glutamine deprivation on tumor growth related factors expression in U87 glioma cells

ERN1 modifies the effect of glutamine deprivation on tumor growth related factors expression in U87 glioma cells

The impact of glutamine deprivation on the expression of MEIS3, SPAG4, LHX1, LHX2, and LHX6 genes in ERN1 knockdown U87 glioma cells

General Transcription Factor IIF Polypeptide 2: A Novel Therapeutic Target for Depression Identified Using an Integrated Bioinformatic Analysis

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