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Query: UMLS:C0017638 (
glioma
)
30,880
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Scatter factor (SF) (also known as hepatocyte growth factor [
HGF
]) is a cytokine that induces cell motility in vitro and angiogenesis in vivo. SF appears to be a determinant of the malignant phenotype in certain systemic cancers. We detected SF in extracts prepared from human gliomas, with the highest levels found in malignant tumors. Human glioblastoma cells expressed both SF and its receptor (c-met protein) in vivo, as demonstrated by immunohistochemistry. Consistent with these observations, we found moderate to high levels of production of immunoreactive and biologically active SF by cultured human glioblastoma cells (3 of 8 lines) and by neural microvascular endothelial cells (NMVEC) (3 of 3 lines). SF stimulated the proliferation of glioblastoma and NMVEC cell lines by paracrine or autocrine mechanisms. Conditioned medium (CM) from both glioblastoma and NMVEC cells contained SF-inducing factor (SF-IF) activity, defined by its ability to stimulate SF production in an indicator cell line (MRC5 human fibroblasts). This activity consisted of a high-molecular-weight (> 30 kDa), heat-sensitive component and a low-molecular weight (< 30 kDa), heat-stable component. Furthermore, glioblastoma CM stimulated NMVEC SF production, and NMVEC CM stimulated glioblastoma cell SF production, by 3- to 6-fold in each case. Our findings demonstrate that SF-dependent interactions between
glioma
cells, and between
glioma
cells and endothelium, can contribute to the heterogeneous proliferative and angiogenic phenotypes of malignant gliomas in vivo.
...
PMID:Scatter factor expression and regulation in human glial tumors. 876 May 95
Using double immunofluorescence staining and quantitative confocal laser scan microscopy, we show that the intensity of hepatocyte growth factor/scatter factor (
HGF
/SF) and Met staining in human primary brain tumors increases with the grade of malignancy and is prevalent in both the infiltrating tumor cells and endothelial hyperplastic areas.
HGF
/SF and Met also are expressed in vitro in glioblastoma multiforme cell lines as well as in normal human astrocyte (NHA) cells. Moreover,
HGF
/SF stimulates tyrosine phosphorylation of Met in both
glioma
cell lines and NHA cells, but only the
glioma
cell lines proliferate and become motile and invasive in response to
HGF
/SF, whereas the NHA cells are nonresponsive. These results implicate autocrine/paracrine Met-
HGF
/SF signaling in
glioma
tumorigenesis and suggest that
HGF
/SF signaling through Met is negatively regulated in NHA cells.
...
PMID:Met and hepatocyte growth factor/scatter factor expression in human gliomas. 939 65
Hepatocyte growth factor/scatter factor (
HGF
/SF) is a mesenchyme-derived cytokine that stimulates motility and invasiveness of epithelial and cancer cells. These responses are transduced through the c-met proto-oncogene product, a transmembrane tyrosine kinase that functions as the HGF/SF receptor. We have shown that
HGF
/SF is a potent angiogenic molecule and that its angiogenic activity is mediated primarily through direct actions on vascular endothelial cells. These include stimulation of cell migration, proliferation, protease production, invasion, and organization into capillary-like tubes. We further showed that
HGF
/SF is overexpressed in invasive human cancers, including breast cancer, relative to non-invasive cancers and benign conditions. In invasive breast cancers, the content of
HGF
/SF is strongly correlated with that of von Willebrand's factor, a marker of vascular endothelial cells. Furthermore, transfection of breast cancer and
glioma
cell lines with
HGF
/SF cDNA greatly enhanced the ability of these cells to grow as tumours in orthotopic sites in syngeneic or immunocompromized host animals. The increased growth rate of the
HGF
/SF-transfected cells was attributable, in part, to increased tumour angiogenesis. These findings suggest that
HGF
/SF may function as a tumour progression factor, in part by stimulating tumour cell invasiveness and in part by stimulating angiogenesis.
...
PMID:HGF/SF in angiogenesis. 952 73
Hepatocyte growth factor/scatter factor (
HGF
/SF), which has various physiological functions, and its receptor c-Met, the human c-met proto-oncogene product, are thought to be determinant in the pathological processes of various malignancies. To investigate the possible role of
HGF
/SF in the progression of development of astrocytic tumors, we examined the expression of c-Met in these tumors. Immunohistochemistry using the streptavidin-biotin peroxidase complex method and immunofluorescence double staining with anti-c-Met polyclonal and anti-glial fibrillary acidic protein monoclonal antibodies were performed. Positive c-Met expression was detected in 31 of the 42 astrocytic tumors and some of the control cases analyzed. c-Met-positive cells showed morphological characteristics of astrocytes. Especially in the cases of high-grade tumors, c-Met positivity was abundant in cells in both vascular-rich and peripheral regions of the tumors but not in the cells with distinctly malignant features. Immunofluorescence double staining revealed that the c-Met-positive cells were in part of astrocytic origin. We suggest that c-Met-positive cells are affected by some factors in the lesions where the pathological processes are in a state of development. Our studies indicated that c-Met expression might take part in
glioma
invasion but not in the development of malignancy.
...
PMID:Immunohistochemical examination of c-Met protein expression in astrocytic tumors. 956 11
Recent findings suggest that hepatocyte growth factor/scatter factor (
HGF
/SF) contributes to the malignant progression of human gliomas. We investigated the effect of
HGF
/SF on vascular endothelial growth factor (VEGF) expression of c-Met/HGF receptor-positive human
glioma
cell lines. Treatment of the
glioma
cells with various concentrations of
HGF
/SF resulted in an enhanced secretion of VEGF proteins accompanying increased transcription of VEGF mRNA in a dose-dependent fashion. Since malignant gliomas frequently co-express
HGF
/SF and its receptor, these results suggest that
HGF
/SF could act as an indirect angiogenic factor through autocrine induction of VEGF expression and secretion in malignant gliomas.
...
PMID:Up-regulation of vascular endothelial growth factor induced by hepatocyte growth factor/scatter factor stimulation in human glioma cells. 970 34
Angiogenesis is a possible target in the treatment of human gliomas. To evaluate the role of 3 growth factors, vascular endothelial growth factor (VEGF), hepatocyte growth factor/scatter factor (
HGF
/SF) and basic fibroblast growth factor (bFGF), in the angiogenic cascade, we determined their levels in extracts of 71 gliomas by enzyme-linked immunosorbent assay (ELISA). The levels of bFGF were only marginally different between gliomas of World Health Organization (WHO) grade II (low grade) and grades III and IV (high grade). In contrast, the mean concentrations of VEGF were 11-fold higher in high-grade tumors and those of
HGF
/SF 7-fold, respectively. Both were highly significantly correlated with microvessel density (p < 0.001) as determined by immunostaining for factor VIII-related antigen. In addition, VEGF and
HGF
/SF appeared to be independent predictive parameters for
glioma
microvessel density as determined by multiple regression analysis. We measured the capacity of all 3 factors to induce endothelial tube formation in a collagen gel. In this assay, bFGF was found to be an essential cofactor with which VEGF as well as
HGF
/SF were able to synergize independently. According to the concentrations of angiogenic factors, extracts from high-grade tumors were significantly more potent in the tube formation assay than the low-grade extracts (p = 0.02). Adding neutralizing antibodies to bFGF, VEGF and
HGF
/SF together with the extracts, tube formation was inhibited by up to 98%, 62% and 54%, respectively. Our findings suggest that bFGF is an essential cofactor for angiogenesis in gliomas, but in itself is insufficient as it is present already in the sparsely vascularized low-grade tumors. Upon induction of angiogenesis in high-grade tumors, bFGF may synergize with rising levels of not only VEGF but possibly also with
HGF
/SF, which appears here to be an independent angiogenic factor.
...
PMID:Levels of vascular endothelial growth factor, hepatocyte growth factor/scatter factor and basic fibroblast growth factor in human gliomas and their relation to angiogenesis. 998 25
Malignant gliomas are associated with a dysfunctional blood-tumor barrier (BTB) that causes substantial morbidity. Scatter factor/hepatocyte growth factor (SF/
HGF
) is a multifunctional growth factor that correlates with
glioma
malignancy and has several biological properties that suggest a role in enhancing blood-
glioma
barrier permeability. In this study, we examined the effects of
glioma
cell SF/
HGF
expression on BTB permeability to horseradish peroxidase (HRP). Fischer 344 rats bearing intrastriatal 9L tumors engineered to secrete SF/
HGF
(9L-SF) and SF/
HGF
-negative control tumors (9L-neo) received intracardiac injections of HRP and were rapidly decapitated. Densitometric analysis of brain sections reacted with diaminobenzidine showed significantly greater extravascular HRP surrounding SF/
HGF
-secreting tumors than 9L-neo tumors of comparable size (p<0.05). HRP enzymatic activity associated with striata containing SF/
HGF
-expressing tumors was 1. 6-fold greater than that of striata containing control tumors (p<0. 05). Northern analysis showed that expression of vascular endothelial growth factor/vascular permeability factor (VEGF/VPF) did not differ between 9L-neo and 9L-SF tumors. These data demonstrate that SF/
HGF
expression by intracerebral
glial tumors
can enhance BTB permeability independent of changes in VEGF/VPF expression.
...
PMID:Scatter factor/hepatocyte growth factor gene transfer increases rat blood-glioma barrier permeability. 1037 92
Hepatocyte growth factor/scatter factor (
HGF
/SF) contributes to the malignant progression of human gliomas. We investigated the effect of
HGF
/SF on matrix metalloproteinase-2 (MMP-2), membrane type 1 matrix metalloproteinase (MT1-MMP) and tissue inhibitors of metalloproteinases (TIMPs), expressions of c-Met/HGF receptor-positive human glioblastoma cells. Treatment of U251 human glioblastoma cells with
HGF
/SF resulted in enhanced secretion of MMP-2 with an increased level of the active form. This was accompanied by enhanced expression (2.5-fold) of mRNA specific for MMP-2. The stimulatory effect of
HGF
/SF on MMP-2 expression did not occur in the presence of herbimycin A, a protein tyrosine kinase inhibitor. MT1 -MMP, a cell-surface activator of proMMP-2, was also up-regulated by
HGF
/SF in a dose-dependent manner. By contrast, the level of TIMP- 1 mRNAs was not altered significantly and that of TIMP-2 was reduced mildly by the
HGF
/SF treatment, suggesting that
HGF
/SF may eventually modulate a balance between MMP-2 and TIMPs in favor of the proteinase activity in the
glioma
cell microenvironment.
HGF
/SF also stimulated MMP-2 expression of other glioblastoma cell lines. Since glioblastomas frequently co-express
HGF
/SF and its receptor, our results suggest that
HGF
/SF might contribute to the invasiveness of glioblastoma cells through autocrine induction of MMP-2 expression and activation.
...
PMID:Regulation of matrix metalloproteinase-2 (MMP-2) by hepatocyte growth factor/scatter factor (HGF/SF) in human glioma cells: HGF/SF enhances MMP-2 expression and activation accompanying up-regulation of membrane type-1 MMP. 1038 63
Scatter factor/hepatocyte growth factor (SF/
HGF
) is a pleiotrophic cytokine that stimulates motility and invasion of several cancer cell types and induces angiogenesis. Its receptor MET is a transmembrane tyrosine kinase encoded by the C-MET proto-oncogene. To assess the potential relevance of SF/
HGF
in gliomas we performed functional studies in vivo and in vitro, expression analyses and correlative studies. We showed that both SF/
HGF
and MET are expressed in gliomas in vivo and are upregulated during transition from low grade to malignant
glioma
. When SF/
HGF
cDNA was transfected into
glioma
cells that expressed the MET receptor the cells formed considerably larger and more vascularized intracranial tumors in vivo than SF/
HGF
negative control clones. In other
glioma
cells, which constitutively expressed both SF/
HGF
and MET, we abolished SF/
HGF
expression by antisense ribozyme-targeting, which led to a significant decrease in tumorigenicity and tumor growth. In vitro SF/
HGF
strongly stimulated
glioma
cell motility and to a lesser degree proliferation. SF/
HGF
also strongly increased endothelial cell motility in vitro and extracts of tumors derived from SF/
HGF
-transfected
glioma
cells were more mitogenic for endothelial cells and more angiogenic in the rat cornea angiogenesis assay than extracts from control tumors. In a three-dimensional in vitro angiogenesis assay basic fibroblast growth factor (bFGF) was found to synergize with either SF/
HGF
or vascular endothelial growth factor (VEGF) in inducing endothelial capillary-like tubes, whereas neither SF/
HGF
nor VEGF alone or in combination were effective. Interestingly, while both VEGF and SF/
HGF
levels appeared to be increased in malignant gliomas compared with low grade ones, this was not the case for bFGF of which biologically relevant levels were already present in low grade gliomas. It thus seems that bFGF alone is insufficient to induce angiogenesis in gliomas but may act synergistically with either VEGF and/or SF/
HGF
when these become upregulated during malignant progression. In conclusion, we showed that SF/
HGF
may contribute to
glioma
progression by stimulating tumor invasiveness, proliferation and neovascularization.
...
PMID:Scatter factor/hepatocyte growth factor (SF/HGF) content and function in human gliomas. 1057 13
Strategies that antagonize growth factor signaling are attractive candidates for the biological therapy of brain tumors.
HGF
/NK2 is a secreted truncated splicing variant and potential antagonist of scatter factor/hepatocyte growth factor (SF/
HGF
), a multifunctional cytokine involved in the malignant progression of solid tumors including glioblastoma. U87 human malignant
glioma
cells that express an autocrine SF/
HGF
stimulatory loop were transfected with the human
HGF
/NK2 cDNA and clonal cell lines that secrete high levels of
HGF
/NK2 protein (U87-NK2) were isolated. The effects of
HGF
/NK2 gene transfer on the U87 malignant phenotype were examined.
HGF
/NK2 gene transfer had no effect on 2-dimensional anchorage-dependent cell growth. In contrast, U87-NK2 cell lines were approximately 20-fold less clonogenic in soft agar and approximately 4-fold less migratory than control-transfected cell lines. Intracranial tumor xenografts derived from U87-NK2 cells grew much slower than controls. U87-NK2 tumors were approximately 50-fold smaller than controls at 21 days post-implantation and
HGF
/NK2 gene transfer resulted in a trend toward diminished tumorigenicity. This report shows that the predominant effect of transgenic
HGF
/NK2 overexpression by
glioma
cells that are autocrine for SF/
HGF
stimulation is to inhibit their malignant phenotype.
...
PMID:Glioma inhibition by HGF/NK2, an antagonist of scatter factor/hepatocyte growth factor. 1087
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