Malignant gliomas display altered pH regulation by NHE1 compared with nontransformed astrocytes

McLean, Lee Anne; Roscoe, Jane; Jørgensen, Nanna K.; Gorin, Fredric A; Cala, Peter M

doi:10.1152/ajpcell.2000.278.4.c676

Cited by 177 publications

(160 citation statements)

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“…Dopa decarboxylase (DDC) is responsible for the synthesis of the key neurotransmitters dopamine and serotonin, and is frequently expressed in neuroblastoma and small cell carcinoma of the lung (North and Du, 1998;Gilbert et al, 1999). Sodium/ hydrogen exchanger isoform 1, is activated more in malignant gliomas than nontransformed astrocytes, and malignant gliomas display altered pH regulation (Lagana et al, 2000;McLean et al, 2000). LMO7 in gastric cancer has not been dealt with in any reports, but another isoform, LMO4 (a transcriptional regulator) inhibits differentiation of mammary epithelial cells in vitro and is GenBank accession number, fold change verified by high-density oligonucleotide array and Northern blot, and one representative function of the genes as previously reported are shown.…”

Section: Genes Related To Signalling (Growth and Metabolism)mentioning

confidence: 99%

Differential gene expression profiles of gastric cancer cells established from primary tumour and malignant ascites

et al. 2002

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Advanced gastric cancer is often accompanied by metastasis to the peritoneum, resulting in a high mortality rate. Mechanisms involved in gastric cancer metastasis have not been fully clarified because metastasis involves multiple steps and requires a combination of altered expressions of many different genes. Thus, independent analysis of any single gene would be insufficient to understand all of the aspects of gastric cancer peritoneal dissemination. In this study, we performed a global analysis of the differential gene expression of a gastric cancer cell line established from a primary main tumour (SNU-1) and of other cell lines established from the metastasis to the peritoneal cavity (SNU-5, SNU-16, SNU-620, KATO-III and GT3TKB). The application of a high-density cDNA microarray method made it possible to analyse the expression of approximately 21 168 genes. Our examinations of SNU-5, SNU-16, SNU-620, KATO-III and GT3TKB showed that 24 genes were upregulated and 17 genes down-regulated besides expression sequence tags. The analysis revealed the following altered expression such as: (a) up-regulation of CD44 (cell adhesion), keratins 7, 8, and 14 (epitherial marker), aldehyde dehydrogenase (drug metabolism), CD9 and IP3 receptor type3 (signal transduction); (b) down-regulation of IL2 receptor g, IL4-Stat (immune response), p27 (cell cycle) and integrin b4 (adhesion) in gastric cancer cells from malignant ascites. We then analysed eight gastric cancer cell lines with Northern blot and observed preferential up-regulation and down-regulation of these selected genes in cells prone to peritoneal dissemination. Reverse transcriptase -polymerase chain reaction confirmed that several genes selected by DNA microarray were also overexpressed in clinical samples of malignant ascites. It is therefore considered that these genes may be related to the peritoneal dissemination of gastric cancers. The results of this global gene expression analysis of gastric cancer cells with peritoneal dissemination, promise to provide a new insight into the study of human gastric cancer peritoneal dissemination.

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Section: Genes Related To Signalling (Growth and Metabolism)mentioning

confidence: 99%

Differential gene expression profiles of gastric cancer cells established from primary tumour and malignant ascites

et al. 2002

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“…The ubiquitously expressed Na þ /H þ exchanger isoform, sodium hydrogen exchanger (NHE1), also contributes to this acidic environment (Plopper et al, 1995). NHE1 activity is important for many tumor cells (Lagarde et al, 1988;Rotin et al, 1989;McLean et al, 2000). Insufficient and/ or inefficient tumor vascularization leads to diminished O 2 supply so that tumor cell metabolism is mostly glycolytic (Helmlinger et al, 2002).…”

Section: Introductionmentioning

confidence: 99%

BAX inhibitor-1 enhances cancer metastasis by altering glucose metabolism and activating the sodium-hydrogen exchanger: the alteration of mitochondrial function

Shin

et al. 2010

Oncogene

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The anti-apoptotic protein, BAX inhibitor-1 (BI-1), has a role in cancer/tumor progression. BI-1-overexpressing HT1080 and B16F10 cells produced higher lung weights and tumor volumes after injection into the tail veins of mice. Transfection of BI-1 siRNA into cells before injection blocked lung metastasis. in vitro, the overexpression of BI-1 increased cell mobility and invasiveness, with highly increased glucose consumption and cytosolic accumulation of lactate and pyruvate, but decreased mitochondrial O 2 consumption and ATP production. Glucose metabolism-associated extracellular pH also decreased as cells excreted more H þ , and sodium hydrogen exchanger (NHE) activity increased, probably as a homeostatic mechanism for intracellular pH. These alterations activated MMP 2/9 and cell mobility and invasiveness, which were reversed by the NHE inhibitor, 5-(N-ethyl-N-isopropyl) amiloride (EIPA), suggesting a role for NHE in cancer metastasis. In both in vitro and in vivo experiments, C-terminal deleted (CDBI-1) cells showed similar results to control cells, suggesting that the C-terminal motif is required for BI-1-associated alterations of glucose metabolism, NHE activation and cancer metastasis. These findings strongly suggest that BI-1 reduces extracellular pH and regulates metastasis by altering glucose metabolism and activating NHE, with the C-terminal tail having a pivotal role in these processes.

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“…However, further studies are needed to determine whether or not the intervention of antisense NHE1 gene can decrease type 1 Na + /H + exchanger of membranous ion exchange protein in gastric carcinoma cells and reverse the malignant phenotypes. Therefore, in the present study, the purpose of transfection of antisense NHE1 gene into human gastric carcinoma cell line [19][20][21][22][23][24][25][26] . The enhancement of Na + -H + exchange by tumor cells, caused by increasing the quantitative distribution of NHE1 on the cell membrane, is the major molecular mechanism in the regulation of pH i in tumor cells.…”

Section: Discussionmentioning

confidence: 99%

Effect of NHE1 antisense gene transfection on the biological behavior of SGC-7901 human gastric carcinoma cells

Liu¹,

Teng²,

Zheng³

et al. 2008

WJG

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AIM:To study the effect of type 1 Na + /H + exchanger (NHE1 ) antisense human gene transfection on the biological behavior of gastric carcinoma cell line SGC-7901. METHODS:Antisense NHE1 eukaryotic expression on vector pcDNA3.1 was constructed by recombinant DNA technique and transfected into gastric carcinoma cell line SGC-7901 with DOTAP liposome transfection method.Morphological changes of cells were observed with optic and electron microscopes. Changes in cell proliferative capacity, apoptosis, intracellular pH (pHi), cell cycle, clone formation in two-layer soft agar, and tumorigenicity in nude mice were examined. RESULTS:Antisense eukaryotic expressing vectors were successfully constructed and transfected into SGC-7901 . The transfectant obtained named 7901 -antisense (7901-AS ) stablely produced antisense NHE1 . There was a significant difference between the pHi of 7901-AS cells (6.77 ± 0.05) and that of 7901-zeo cells and SGC-7901 cells (7.24 ± 0.03 and 7.26 ± 0.03, P < 0.01). Compared with SGC-7901 and 7901-zeo cells, 7901-AS cells mostly showed cell proliferation inhibition, G1/G0 phase arrest, increased cell apoptotic rate, recovery of contact inhibition, and density contact. The tumorigenicity in nude mice and cloning efficiency in the two-layer soft agar were clearly inhibited.

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Malignant gliomas display altered pH regulation by NHE1 compared with nontransformed astrocytes

Cited by 177 publications

References 50 publications

Differential gene expression profiles of gastric cancer cells established from primary tumour and malignant ascites

Differential gene expression profiles of gastric cancer cells established from primary tumour and malignant ascites

BAX inhibitor-1 enhances cancer metastasis by altering glucose metabolism and activating the sodium-hydrogen exchanger: the alteration of mitochondrial function

Effect of NHE1 antisense gene transfection on the biological behavior of SGC-7901 human gastric carcinoma cells

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