3rd International Conference on Osteopontin and SIBLING (Small Integrin-Binding Ligand, N-Linked Glycoprotein) Proteins, 2002 2002
DOI: 10.1100/tsw.2002.247
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Promotion of Malignant Astrocytoma Cell Migration by Osteopontin Expressed in the Normal Brain: Differences in Integrin Signaling During Cell Adhesion to Osteopontin vs. Vitronectin

Abstract: The extracellular matrix of the normal adult brain lacks expression of most of the adhesive glycoproteins that are known to promote cell attachment, and it has been thought that the malignant invasion of astrocytoma tumor is mediated primarily by remodeling of the matrix by the tumor cells. It has been reported, however, that normal brain neuropil does contain a protein(s) that promotes cell attachment. Therefore, we explored the possibility that the cell attachment protein, osteopontin, is expressed in the no… Show more

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Cited by 61 publications
(78 citation statements)
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“…FAK overexpression has been shown to promote invasion of A549 lung adenocarcinoma cells and of v-Src-transformed fibroblasts through Matrigel (Sieg et al, 2000;Brabek et al, 2004). Using an invasion assay into detergent-free normal brain homogenate as we have described previously (Ding et al, 2002), we found a twofold increase in invasion of doxycyclinetreated OFAK5 cells as compared to cells administered Figure 1 FAK promotes PDGF-stimulated migration of glioblastoma cells adherent to rec-osteopontin. OFAK5 cells were treated with 2 mg/ml doxycycline or vehicle for 2 days in DMEM-10% FBS, replated onto rec-osteopontin in DMEM-0.4% FBS-1% BSA, and treated with 1 mg/ml doxycycline or vehicle for 2 days.…”
Section: Fak Promotes Invasion Of Glioblastoma Cells Through Detergensupporting
confidence: 54%
See 1 more Smart Citation
“…FAK overexpression has been shown to promote invasion of A549 lung adenocarcinoma cells and of v-Src-transformed fibroblasts through Matrigel (Sieg et al, 2000;Brabek et al, 2004). Using an invasion assay into detergent-free normal brain homogenate as we have described previously (Ding et al, 2002), we found a twofold increase in invasion of doxycyclinetreated OFAK5 cells as compared to cells administered Figure 1 FAK promotes PDGF-stimulated migration of glioblastoma cells adherent to rec-osteopontin. OFAK5 cells were treated with 2 mg/ml doxycycline or vehicle for 2 days in DMEM-10% FBS, replated onto rec-osteopontin in DMEM-0.4% FBS-1% BSA, and treated with 1 mg/ml doxycycline or vehicle for 2 days.…”
Section: Fak Promotes Invasion Of Glioblastoma Cells Through Detergensupporting
confidence: 54%
“…The PDGF-stimulated migration of glioblastoma cells on osteopontin and vitronectin is of interest as the PDGF A and B genes, as well as the PDGFr-a and -b genes, are upregulated in glioblastoma tumors (Hermanson et al, 1992), osteopontin and vitronectin are expressed in glioblastoma tumors, and osteopontin is also expressed in the normal brain (Gladson et al, 1995;Ding et al, 2002). We therefore analysed the role of FAK in the migration of glioblastoma cells using previously described clones of U-251MG glioblastoma cells that overexpress wild-type FAK (clone OFAK5) under the regulation of a TET-inducible promoter (Wang et al, 2000).…”
Section: Fak Promotes Pdgf-stimulated Migration Of Glioblastoma Cellsmentioning
confidence: 99%
“…18 In a recent study, osteopontin was also found to promote the attachment of malignant astrocytoma cells to become more metastasized and invasive. 19 On the basis of our in vitro and in vivo observations, the high expression of OPN in AT/RT may be associated with tumor cell invasion and dissemination, which may lead to the unique clinical character of the disease and poor outcome of AT/RT patients.…”
Section: Discussionmentioning
confidence: 87%
“…These observations, combined with low expression levels in benign tumors, suggest that OPN dysregulation is important in cell transformation or that elevated OPN expression contributes to malignant and metastatic character. In the brain OPN is intimately associated with the extracellular matrix (ECM) and its expression is developmentally regulated, suggesting that it may facilitate neuronal or glial cell migration [12,29]. Consistent with its role in the stress response, OPN has been implicated as a possible mediator of CNS inflammatory diseases, as a neuroprotective agent in acute stroke and is up-regulated in models of CNS degenerative disease and epilepsy [6,22,35].…”
Section: Introductionmentioning
confidence: 99%