Glutamate Promotes Cell Growth by EGFR Signaling on U-87MG Human Glioblastoma Cell Line

Schunemann, Daniel Pretto; Grivicich, Ivana; Regner, Andréa; Leal, Lisiane Freitas; Araújo, Daniela Romani de; Jotz, Geraldo Pereira; Fedrigo, Carlos Alexandre; Simon, Daniel; Rocha, Adriana Brondani da

doi:10.1007/s12253-009-9223-4

Cited by 28 publications

(32 citation statements)

References 59 publications

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“…The (glutamate-glutamine)-to-creatine ratio in patients with GBM agrees with reports of higher levels of glutamate in the tumor than in peritumoral tissue ( 5 ), which is consistent with reports that GBM secretes large amounts of glutamate ( 38,39 ).…”

Section: Discussionsupporting

confidence: 91%

Use of in Vivo Two-dimensional MR Spectroscopy to Compare the Biochemistry of the Human Brain to That of Glioblastoma

Ramadan¹,

Andronesi²,

Stanwell³

et al. 2011

Radiology

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Localized correlation spectroscopy of the human brain at 3.0 T with use of a 32-channel head coil was performed in 11 minutes and provided information about neurotransmitters, metabolites, lipids, and macromolecules. The method was able to help differentiate healthy brain from the biochemical signature of GBM in vivo. This method may, in the future, reduce the need for biopsy and is now applicable for the study of selected neurologic diseases.

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Section: Discussionsupporting

confidence: 91%

Use of in Vivo Two-dimensional MR Spectroscopy to Compare the Biochemistry of the Human Brain to That of Glioblastoma

Ramadan¹,

Andronesi²,

Stanwell³

et al. 2011

Radiology

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“…Moreover, recurrent glioblastomas are resistant to conventional radiotherapy and chemotherapy. Many cell adhesion proteins, cytoplasmic proteins and growth factor receptors, including the neural cell adhesion molecule (NCAM), matrix metalloproteinase (MMP), integrin, CD44 and epidermal growth factor receptor (EGFR), play important roles in glioblastoma cell migration and invasion (4)(5)(6). These factors affect the intracellular states of tumor cells and induce their migration and invasion.…”

Section: Introductionmentioning

confidence: 99%

Neuroepithelial stem cell marker nestin regulates the migration, invasion and growth of human gliomas

Ishiwata

Teduka²,

Yamamoto³

et al. 2011

Oncol Rep

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Abstract. Nestin, a class VI intermediate filament protein, was originally described as a neuronal stem cell marker during central nervous system development. Nestin is expressed in gliomas, and its expression levels are higher in gliomas with high WHO histopathological classification grades than in those with low grades. In the present study, we examined whether nestin regulates the biological activities of human glioma cells. Immunohistochemically, the nestin expression patterns in 10 human glioblastoma patients were examined. The expression levels of nestin in A172, a human high-grade glioma cell line, and KG-1-C, a human low-grade glioma cell line, were examined using real-time PCR, Western blot and immunofluorescence analyses. An expression vector carrying a short hairpin RNA targeting nestin was stably transfected into A172 (Sh) cells. The effects of decreased expression levels of nestin in Sh cells on cell growth, migration, invasion, adhesion to extracellular matrices and fibrillar actin expression on three-dimensional culture plates were examined. The nestin expression vector was transiently transfected into KG-1-C (Nes) cells, and the effects of the nestin overexpression on cell growth and migration were examined. Nestin was expressed in the cytoplasm of the glioblastoma cells in all cases examined. Sh cells showed marked decreases in the expression levels of nestin mRNA and protein, and the growth rate of Sh cells was lower than that of sham (Sc) cells. In contrast, the adhesion activity of Sh cells to types I and IV collagens, fibronectin and laminin was higher than that of Sc cells. Fibrillar actin was clearly detected at the periphery of colonies of Sh cells at the attachment sites on three-dimensional culture plates. The migration and invasion of Sh cells were markedly inhibited compared with those of Sc cells. In contrast, the levels of nestin expression markedly increased in the Nes cells, which were transiently transfected with the nestin expression vector. The growth rate and motility of Nes cells were higher than those of the mock cells. In conclusion, nestin plays important roles in cell growth, migration, invasion and adhesion to extra-cellular matrices in glioma cells. Nestin may serve as a novel candidate for molecular-targeted therapy for gliomas, including glioblastomas.

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“…AMPA receptors on BTICs are comprised of GluR1 and GluR4 subunits (Oh et al 2012), whereas AMPA receptors on the glioblastoma cell line U87MG contain the GluR2 subunit and are Ca 2+ impermeable (Ekici et al 2012). Human surgical glioma tissues contain Ca 2+ permeable AMPA receptors, and glutamate activation promotes cell growth and mobility (Lyons et al 2007) by activation of the Akt pathway (Ishiuchi et al 2007;Schunemann et al 2010). …”

Section: Excessive Glutamate Facilitates Glioma Cell Survival and Promentioning

confidence: 99%

The Role of Inflammation in Brain Cancer

Sowers

Johnson

Conrad

et al. 2014

Advances in Experimental Medicine and Biology

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Malignant brain tumors are among the most lethal of human tumors, with limited treatment options currently available. A complex array of recurrent genetic and epigenetic changes has been observed in gliomas that collectively result in derangements of common cell signaling pathways controlling cell survival, proliferation, and invasion. One important determinant of gene expression is DNA methylation status, and emerging studies have revealed the importance of a recently identified demethylation pathway involving 5-hydroxymethylcytosine (5hmC). Diminished levels of the modified base 5hmC is a uniform finding in glioma cell lines and patient samples, suggesting a common defect in epigenetic reprogramming. Within the tumor microenvironment, infiltrating immune cells increase oxidative DNA damage, likely promoting both genetic and epigenetic changes that occur during glioma evolution. In this environment, glioma cells are selected that utilize multiple metabolic changes, including changes in the metabolism of the amino acids glutamate, tryptophan, and arginine. Whereas altered metabolism can promote the destruction of normal tissues, glioma cells exploit these changes to promote tumor cell survival and to suppress adaptive immune responses. Further understanding of these metabolic changes could reveal new strategies that would selectively disadvantage tumor cells and redirect host antitumor responses toward eradication of these lethal tumors.

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Glutamate Promotes Cell Growth by EGFR Signaling on U-87MG Human Glioblastoma Cell Line

Cited by 28 publications

References 59 publications

Use of in Vivo Two-dimensional MR Spectroscopy to Compare the Biochemistry of the Human Brain to That of Glioblastoma

Use of in Vivo Two-dimensional MR Spectroscopy to Compare the Biochemistry of the Human Brain to That of Glioblastoma

Neuroepithelial stem cell marker nestin regulates the migration, invasion and growth of human gliomas

The Role of Inflammation in Brain Cancer

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