2013
DOI: 10.1186/1471-2407-13-597
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High epiregulin expression in human U87 glioma cells relies on IRE1α and promotes autocrine growth through EGF receptor

Abstract: BackgroundEpidermal growth factor (EGF) receptors contribute to the development of malignant glioma. Here we considered the possible implication of the EGFR ligand epiregulin (EREG) in glioma development in relation to the activity of the unfolded protein response (UPR) sensor IRE1α. We also examined EREG status in several glioblastoma cell lines and in malignant glioma.MethodsExpression and biological properties of EREG were analyzed in human glioma cells in vitro and in human tumor xenografts with regard to … Show more

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Cited by 100 publications
(168 citation statements)
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“…It is important for evaluation of possible signifi cance of these genes in the control of glioma growth through ER stress signaling mediated by IRE1 and hypoxia. It is known that stress signaling pathways are involved in numerous metabolic pathways and inhibition of the activity of IRE1 signaling enzyme in glioma cells had antitumor eff ects (Auf et al 2010(Auf et al , 2013Manie et al 2014;Minchenko et al 2015).…”
Section: Discussionmentioning
confidence: 99%
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“…It is important for evaluation of possible signifi cance of these genes in the control of glioma growth through ER stress signaling mediated by IRE1 and hypoxia. It is known that stress signaling pathways are involved in numerous metabolic pathways and inhibition of the activity of IRE1 signaling enzyme in glioma cells had antitumor eff ects (Auf et al 2010(Auf et al , 2013Manie et al 2014;Minchenko et al 2015).…”
Section: Discussionmentioning
confidence: 99%
“…Th e changes in these genes expression in cells without IRE1 signaling enzyme function possible contribute in the suppression of glioma cell proliferation and tumor growth, because there are data indicating that the estrogen receptor related factors play an important role in the control of cell proliferation and apoptosis (Cho et al 2010;Lapierre et al 2015;Tiwari et al 2015). It is possible that increased expression of FAM162A, PGRMC2, TRIM16 and SLC39A6 genes as well as decreased expression of ESRRA, and NRIP1 genes (Figure 1) may contribute to the suppression of the proliferation and glioma growth from glioma cells with IRE1 knockdown (Auf et al 2010(Auf et al , 2013Aziz et al 2015;Casaburi et al 2015;Minchenko et al 2015;Zhang et al 2015;Matsushima et al 2016). Th erefore, suppressing of NRIP1, which modulates transcriptional activity of the estrogen receptor, as well as knockdown of a site-specifi c transcription regulator ESRRA/NR3B1 inhibits growth of the cancer cells in vitro and in vivo (Aziz et al 2015;Matsushima et al 2016).…”
Section: Discussionmentioning
confidence: 99%
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“…Both domains contributed to ERN1 signaling [30]. The IRE1as sociated protein kinase autophosphorylates and di merizes this enzyme in the endoplasmic reticulum membrane, leading to the activation of its endoribo nuclease domain, and has some additional functions [7]. Endoribonuclease activity is responsible for deg radation of a specific subset of mRNA and initiation of the preXBP1 (Xbox binding protein 1) mRNA splicing that stimulates the expression of more than five hundreds of unfolded protein response-specific genes [6,30,31].…”
Section: We Have Studied the Effect Of Hypoxia On The Expression Levementioning
confidence: 99%