Ganglioside GD1a inhibits HGF-induced motility and scattering of cancer cells through suppression of tyrosine phosphorylation of c-Met

Hyuga, Sumiko; Kawasaki, Nana; Hyuga, Masashi; Ohta, Miyako; Shibayama, Rie; Kawanishi, Toru; Yamagata, Sadako; Yamagata, Toshio; Hayakawa, Tetsuo

doi:10.1002/ijc.1481

Cited by 26 publications

(17 citation statements)

References 31 publications

(33 reference statements)

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“…Several studies have reported that exposure to gangliosides can induce the production of various inflammatory mediators such as cytokines (Blennow et al 1991). Ganglioside GD1a has been reported to suppress FBJ cells growth (Hyuga et al 2001). Our find the GD1a expression and synthase was increased in cocultured cells were increased the inflammatory factors such as TNF-α, p65, and p 50.…”

Section: Discussionsupporting

confidence: 55%

Relationship between ganglioside GD1a and inflammatory response in the coculture of human endothelial cells with porcine endothelial cells

Kwak

Lee

et al. 2014

Animal Cells and Systems

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Gangliosides are ubiquitous components of cell membranes that can act as mediators of cell adhesion and signal transduction. However, their interaction with adhesion molecules in vascular grafts following xenotransplantation is not yet clearly understood. In this study, human umbilical vein endothelial cells (HUVECs) were cocultured with porcine aortic endothelial cells (PAECs) in order to investigate the expression patterns of gangliosides, inflammation factors, and the mRNA levels of adhesion molecules by PCR and western blot. The expression of gangliosides GM3 and GM1 was detected in both HUVECs and PAECs, while GD3 was expressed only in PAECs. However, when HUVECs were cocultured with PAECs, GD1a expression was newly detected. In addition, we observed the mRNA expression levels of adhesion molecules including such as E-selectin, intercellular adhesion molecule-1, vascular cell adhesion molecule-1, and platelet endothelial cell adhesion molecule-1 were higher in cocultured HUVECs with PAECs than in either HUVECs or PAECs cultured alone. Furthermore, when HUVECs were cocultured with PAECs, cell growth was significantly inhibited compared with either HUVECs or PAECs. The growth inhibition of both cocultured cells and HUVECs by lipopolysaccharide was significantly increased by GD1a treatment. When HUVECs with PAECs were cocultured, expression of GD1a and inflammatory factors including tumor necrosis factor-α (TNF-α), p65, and p50 significantly increased. These results suggest that GD1a interact with components of the proinflammatory response pathway in xenotransplantation. Therefore, may be relevant for designing future therapeutic strategies intended to prolong xenograft survival.

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Section: Discussionsupporting

confidence: 55%

Relationship between ganglioside GD1a and inflammatory response in the coculture of human endothelial cells with porcine endothelial cells

Kwak

Lee

et al. 2014

Animal Cells and Systems

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“…Previously, it has been shown that a-series gangliosides act as negative regulators of c-Met. G D1a inhibits HGF-induced motility and scattering of cancer cells through suppression of tyrosine phosphorylation of c-Met (33). G M3 and G M2 form heterodimers that specifically interact with tetraspanin (CD82) in glycosynapses, and such complexes inhibit c-Met activation and integrin cross talk (34,35).…”

Section: Discussionmentioning

confidence: 99%

GD3 Synthase Expression Enhances Proliferation and Tumor Growth of MDA-MB-231 Breast Cancer Cells through c-Met Activation

Cazet

Lefebvre

Adriaenssens

et al. 2010

Molecular Cancer Research

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The disialoganglioside G D3 is overexpressed in ∼50% of invasive ductal breast carcinoma, and the G D3 synthase gene (ST8SIA1) displays higher expression among estrogen receptor-negative breast cancer tumors, associated with a decreased overall survival of breast cancer patients. However, no relationship between ganglioside expression and breast cancer development and aggressiveness has been reported. We have previously shown that overexpression of G D3 synthase induces the accumulation of b-and c-series gangliosides (G D3 , G D2 , and G T3 ) at the cell surface of MDA-MB-231 breast cancer cells together with the acquisition of a proliferative phenotype in the absence of serum. Here, we show that phosphoinositide 3-kinase/Akt and mitogen-activated protein kinase/extracellular signal-regulated kinase pathways are constitutively activated in G D3 synthaseexpressing cells. Analysis of phosphorylation of tyrosine kinase receptors shows a specific c-Met constitutive activation in G D3 synthase-expressing cells, in the absence of its ligand, hepatocyte growth factor/scatter factor. In addition, inhibition of c-Met or downstream signaling pathways reverses the proliferative phenotype. We also show that G D3 synthase expression enhances tumor growth in severe combined immunodeficient mice. Finally, a higher expression of ST8SIA1 and MET in the basal subtype of human breast tumors are observed. Altogether, our results show that G D3 synthase expression is sufficient to enhance the tumorigenicity of MDA-MB-231 breast cancer cells through a ganglioside-dependent activation of the c-Met receptor.

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“…LA5-22 cells showed no indication of metastasis in mice to whose thighs these cells had been administered and which were sacrificed at 4 to 5 weeks to confirm the presence of tumor cells in organs macroand microscopically. M5 cells as a control mock transfectant were found to have metastasized to lung, liver and kidney [2]. GD1a is thus shown to control the metastatic machinery of FBJ cells but the underlying mechanism for this remains to be clarified.…”

Section: Introductionmentioning

confidence: 92%

“…Ganglioside GD1a regulates cell motility, cell adhesiveness to vitronectin, phosporylation of c-Met and metastatic capacity of mouse FBJ cell lines [1][2][3]. Using cells derived from FBJ-virus-induced mouse osteosarcoma, FBJ-S1 cells with no indication of metastasis were found to express gangliosides GM3 and GD1a, whereas FBJ-LL cells, capable of mestasizing to lung and liver subsequent to subcutaneous transplantation of cells to mouse thigh, possessed GM3 and GD1a but the latter in only limited amounts.…”

Section: Introductionmentioning

confidence: 99%

Ganglioside GD1a regulation of caveolin-1 and Stim1 expression in mouse FBJ cells:Augmented expression of caveolin-1 and Stim1 in cells with increased GD1a content

et al. 2006

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GD1a was previously shown responsible for regulating cell motility, cellular adhesiveness to vitronectin, phosphorylation of c-Met and metastatic ability of mouse FBJ osteosarcoma cells. To determine the particular molecules regulated by GD1a, FBJ cells were assessed for tumor-related gene expression by semi-quantitative RT-PCR. Caveolin-1 and stromal interaction molecule 1 (Stim1) expression in FBJ-S1 cells, rich in GD1a, were found to be 6 and 4 times as much, respectively, than in FBJ-LL cells devoid of GD1a. Enhanced production of caveolin-1 in protein was confirmed by Western blotting. A low-metastatic FBJ-LL cell variant, having high GD1a expression through beta1-4GalNAcT-1 (GM2/GD2 synthase) cDNA transfection (Hyuga S, et al, Int J Cancer 83: 685-91, 1999), showed enhanced production of caveolin-1 and Stim1 in mRNA and protein, compared to mock-transfectant M5. Incubation of FBJ-M5 cells with exogenous GD1a augmented the expression of caveolin-1 in mRNA and protein and Stim1 in mRNA as well. Treatment of FBJ-S1 with fumonisin B1, an inhibitor of N-acylsphinganine synthesis, for 15 days caused the complete depletion of gangliosides and suppressed the expression of caveolin-1 and Stim1. St3gal5 siRNA transfected cells showed decreased expression of caveolin-1 and Stim1 mRNA, as well as St3gal5 mRNA. These findings clearly indicate ganglioside GD1a to be involved in the regulation of the transformation suppressor genes, caveolin-1 and Stim1. Moreover, treatment with GD1a of mouse melanoma B16 cells and human hepatoma HepG2 cells brought about elevated expression of caveolin-1 and Stim1.

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Ganglioside GD1a inhibits HGF-induced motility and scattering of cancer cells through suppression of tyrosine phosphorylation of c-Met

Cited by 26 publications

References 31 publications

Relationship between ganglioside GD1a and inflammatory response in the coculture of human endothelial cells with porcine endothelial cells

Relationship between ganglioside GD1a and inflammatory response in the coculture of human endothelial cells with porcine endothelial cells

GD3 Synthase Expression Enhances Proliferation and Tumor Growth of MDA-MB-231 Breast Cancer Cells through c-Met Activation

Ganglioside GD1a regulation of caveolin-1 and Stim1 expression in mouse FBJ cells:Augmented expression of caveolin-1 and Stim1 in cells with increased GD1a content

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