1996
DOI: 10.1016/0014-5793(95)01540-x
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Blockage of urokinase receptor reduces in vitro the motility and the deformability of endothelial cells

Abstract: The binding of urokinase (u-PA) to its cell surface receptor (u-PAR) is critical for tumor cell invasion. Here, we report that the disruption of this binding by an u-PAR antagonist ATF-HSA inhibits in vitro the motility of endothelial cells in a dose-dependent manner. This inhibition was also observed when the cells were first stimulated with potent angiogenic factors, including bFGF or VEGF.[3H]thymidine incorporation assay demonstrated that ATF-HSA did not affect the cell proliferation. ATF-HSA was more pote… Show more

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Cited by 49 publications
(31 citation statements)
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“…47,48 It is also considered that such a strategy will benefit from the availability of viral vectors allowing long-term transgene expression to increase efficacy. 49,50 Finally, since activated endothelial cells 5,51 and most solid tumors express uPAR, virus-mediated ATF delivery, alone or in combination therapies with cytotoxic strategies (for example, see Ref. 30), may be particularly potent because this broad cell invasion inhibitor is more than an inhibitor of angiogenesis sensus stricto.…”
Section: Figure 6 Intratumoral Injection Of Admatf Inhibits Llc Tumormentioning
confidence: 99%
See 1 more Smart Citation
“…47,48 It is also considered that such a strategy will benefit from the availability of viral vectors allowing long-term transgene expression to increase efficacy. 49,50 Finally, since activated endothelial cells 5,51 and most solid tumors express uPAR, virus-mediated ATF delivery, alone or in combination therapies with cytotoxic strategies (for example, see Ref. 30), may be particularly potent because this broad cell invasion inhibitor is more than an inhibitor of angiogenesis sensus stricto.…”
Section: Figure 6 Intratumoral Injection Of Admatf Inhibits Llc Tumormentioning
confidence: 99%
“…3 The delivery of a secreted inhibitor of tumor angiogenesis with an adenovirus would thus represent a conceptually different, possibly synergistic, approach to fight cancer. Peptidic angiogenesis inhibitors such as angiostatin, 4 uPA/uPAR antagonists, 5,6 platelet factor-4, 7 or thrombospondin 8 have been described. Among them, the amino-terminal fragment of urokinase (ATF) is of particular interest because it can also exert a direct effect on the tumor cells and inhibit metastasis in experimental models.…”
Section: Introductionmentioning
confidence: 99%
“…The established role of uPA in breast cancer is to proteolytically cleave the extracellular matrix (3). Furthermore, interaction of uPA to uPAR is important for adhesion, motility and migration of cells (4). It was assumed that uPA can exert cytokine-like activity by increasing the proliferation of human epidermal tumor cells and malignant renal cells (5,6).…”
Section: Introductionmentioning
confidence: 99%
“…Conditioned media were incubated in the absence or presence of amino-terminal fragment (ATF) of human urokinase at 200 mM. 25 The medium was renewed every 24 hr. After 4 days, using inverted microscope and focusing deeper into the gel, the number of elongated cells that have migrated into the collagen matrix were counted manually in different conditions and expressed as number of cells per cm 2 .…”
Section: In Vitro Angiogenesis Assaymentioning
confidence: 99%