Expression of merlin, NDRG2, ERBB2, and c-MYC in meningiomas: relationship with tumor grade and recurrence

Ongaratti, Bárbara Roberta; Silva, C.B.O.; Trott, Geraldine; Haag, Taiana; Leães, C.G.S.; Ferreira, Nelson Pires; Oliveira, Miriam C.; Pereira-Lima, Júlia Fernanda Semmelmann

doi:10.1590/1414-431x20155125

Cited by 20 publications

(21 citation statements)

References 39 publications

(62 reference statements)

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“…Although these studies found a strong relationship between loss of NDRG2 expression and tumor grade/recurrence, a larger study by Ongaratti et al (n = 60) did not observe this effect using immunohistochemistry [67]. The lack of reproducibility could have been caused by the small number of meningiomas with invasive and aggressive characteristics in this study (n = 12 for tumor grades II and III combined), or by the fact that the two studies used different antibodies for immunohistochemistry.…”

Section: Meningiomacontrasting

confidence: 62%

Nervous NDRGs: the N-myc downstream–regulated gene family in the central and peripheral nervous system

et al. 2019

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The N-Myc downstream-regulated gene (NDRG) family consists of four members (NDRG1, NDRG2, NDRG3, NDRG4) that are differentially expressed in various organs and function in important processes, like cell proliferation and differentiation. In the last couple of decades, interest in this family has risen due to its connection with several disorders of the nervous system including Charcot-Marie-Tooth disease and dementia, as well as nervous system cancers. By combining a literature review with in silico data analysis of publicly available datasets, such as the Mouse Brain Atlas, BrainSpan, the Genotype-Tissue Expression (GTEx) project, and Gene Expression Omnibus (GEO) datasets, this review summarizes the expression and functions of the NDRG family in the healthy and diseased nervous system. We here show that the NDRGs have a differential, relatively cell typespecific, expression pattern in the nervous system. Even though NDRGs share functionalities, like a role in vesicle trafficking, stress response, and neurite outgrowth, other functionalities seem to be unique to a specific member, e.g., the role of NDRG1 in myelination. Furthermore, mutations, phosphorylation, or changes in expression of NDRGs are related to nervous system diseases, including peripheral neuropathy and different forms of dementia. Moreover, NDRG1, NDRG2, and NDRG4 are all involved in cancers of the nervous system, such as glioma, neuroblastoma, or meningioma. All in all, our review elucidates that although the NDRGs belong to the same gene family and share some functional features, they should be considered unique in their expression patterns and functional importance for nervous system development and neuronal diseases.

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Section: Meningiomacontrasting

confidence: 62%

Nervous NDRGs: the N-myc downstream–regulated gene family in the central and peripheral nervous system

et al. 2019

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“…Wang et al observed that when the gene expression of HER2 was down-regulated, the proliferative and invasive ability of the meningioma cells were decreased, and these cells had higher rates of apoptosis (24). Moreover, consistent with our results, some studies reported the higher expression of HER2 on the surface of higher grade meningiomas, although they stated no statistical significance for this association (14,15). On the other hand, there are studies that report no correlation between HER2 expression and histological grade and prognosis of meningiomas (17,25), and a few studies have even shown decreased HER2 expression in higher grade meningiomas (3).…”

Section: █ Discussionsupporting

confidence: 85%

“…In addition, Wang et al demonstrated that overexpression of HER2 resulted in meningiomas with increased cell invasion, migration, and proliferation, whereas downregulation of HER2 protein expression inhibited the neoplastic cells' motility and proliferation, which led to an increase in apoptosis and arrest cell cycle at the G0/G1-phase (24). In addition, higher expression of HER2 in higher grades of meningioma (grade II, III) in comparison to low-grade tumors (grade I) has been reported (13,15). On the other hand, there are studies that report no association between HER2 expression and meningioma features (14).…”

mentioning

confidence: 99%

Investigating the levels of soluble extracellular domain of her2 protein in the sera of meningioma patients

Abtahi

Hakimrabet²,

Malekzadeh³

et al. 2017

Turkish Neurosurgery

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“…Among the 42 overexpressed genes in our study, the majority (23 of 42) are associated with dysregulation of gene expression in one or more human cancers. These include, but are not limited to, FOSB [ 40 ], FOS [ 41 ], BMPR1B [ 42 ], WNT5A [ 43 , 44 ], PDPN [ 45 ], BMPER [ 46 ], IRF6 [ 47 ], and MYC [ 48 , 49 ]. Additionally, FOS, MYC, and PDPN have been shown to be overexpressed specifically in meningeal tumors [ 41 , 48 , 50 ].…”

Section: Discussionmentioning

confidence: 99%

RNA-seq transcriptome analysis of formalin fixed, paraffin-embedded canine meningioma

et al. 2017

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Meningiomas are the most commonly reported primary intracranial tumor in dogs and humans and between the two species there are similarities in histology and biologic behavior. Due to these similarities, dogs have been proposed as models for meningioma pathobiology. However, little is known about specific pathways and individual genes that are involved in the development and progression of canine meningioma. In addition, studies are lacking that utilize RNAseq to characterize gene expression in clinical cases of canine meningioma. The primary objective of this study was to develop a technique for which high quality RNA can be extracted from formalin-fixed, paraffin embedded tissue and then used for transcriptome analysis to determine patterns of gene expression. RNA was extracted from thirteen canine meningiomas–eleven from formalin fixed and two flash-frozen. These represented six grade I and seven grade II meningiomas based on the World Health Organization classification system for human meningioma. RNA was also extracted from fresh frozen leptomeninges from three control dogs for comparison. RNAseq libraries made from formalin fixed tissue were of sufficient quality to successfully identify 125 significantly differentially expressed genes, the majority of which were related to oncogenic processes. Twelve genes (AQP1, BMPER, FBLN2, FRZB, MEDAG, MYC, PAMR1, PDGFRL, PDPN, PECAM1, PERP, ZC2HC1C) were validated using qPCR. Among the differentially expressed genes were oncogenes, tumor suppressors, transcription factors, VEGF-related genes, and members of the WNT pathway. Our work demonstrates that RNA of sufficient quality can be extracted from FFPE canine meningioma samples to provide biologically relevant transcriptome analyses using a next-generation sequencing technique, such as RNA-seq.

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Expression of merlin, NDRG2, ERBB2, and c-MYC in meningiomas: relationship with tumor grade and recurrence

Cited by 20 publications

References 39 publications

Nervous NDRGs: the N-myc downstream–regulated gene family in the central and peripheral nervous system

Nervous NDRGs: the N-myc downstream–regulated gene family in the central and peripheral nervous system

Investigating the levels of soluble extracellular domain of her2 protein in the sera of meningioma patients

RNA-seq transcriptome analysis of formalin fixed, paraffin-embedded canine meningioma

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