Blockage of the urokinase receptor on the cell surface: Construction and characterization of a hybrid protein consisting of the N‐terminal fragment of human urokinase and human albumin

Lű, He; Yeh, Patrice; Guitton, Jean-Dominique; Mabilat, Christelle; Desanlis, Francine; Maury, Isabelle; Legrand, Yves; Soria, Claudine

doi:10.1016/0014-5793(94)01237-7

Cited by 34 publications

(19 citation statements)

References 24 publications

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“…Invasion assays were carried out in a 12-well Transwell unit (Costar, Cambridge, MA, USA) as described. 11 Briefly, polycarbonate filters of 12 m pore size were coated with 160 g Matrigel (Becton Dickinson France, le Pont-deChaix, France) and dried. The lower chambers of the Transwell units were filled with human fibroblast-conditioned medium containing 10 ng/ml EGF, and the upper chambers were seeded with 3 × 10 5 infected cells.…”

Section: Inhibition Of Cell-associated Proteolysismentioning

confidence: 99%

“…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. [9][10][11] Urokinase and its high affinity receptor, a GPI-anchored membrane protein (CD87), are believed to be critical elements in tumor biology because they control cell motility, tissue remodeling and the bioavailability of angiogenic factors. For example, uPA/uPAR complex formation at the cell surface is required for efficient activation of plasmin, a wide range protease that can degrade components of the basement membrane and the extracellular matrix (eg vitronectin, laminin, fibronectin), a prerequisite for tumor cell invasion.…”

Section: Introductionmentioning

confidence: 99%

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Adenovirus-mediated delivery of a uPA/uPAR antagonist suppresses angiogenesis-dependent tumor growth and dissemination in mice

et al. 1998

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AdmATF is a recombinant adenovirus encoding a secreted within and at the vicinity of the injection site was also supversion of the amino-terminal fragment (ATF) of murine pressed, suggesting that AdmATF inhibited primary tumor urokinase (uPA). This defective adenovirus was used in growth by targeting angiogenesis. AdmATF also interfered three murine models to assess the antitumoral effects with tumor cell establishment at distant sites: (1) lung disassociated with local or systemic delivery of ATF, a broad semination of Lewis lung carcinoma cells was significantly cell invasion inhibitor that antagonizes uPA binding to its reduced following intratumoral injection at the primary site; cell surface receptor (uPAR). A single intratumoral injection and (2) systemic administration of AdmATF inhibited subof AdmATF into pre-established MDA-MB-231 human sequent liver metastasis in a LS174T human colon carcibreast xenografts grown in athymic mice, or into pre-estabnoma xenograft model. These data outline the potential of lished C57/BL6 syngeneic Lewis lung carcinoma resulted using a recombinant adenovirus directing the secretion of an in a specific arrest of tumor growth. Neovascularization antagonist of cell-associated uPA for cancer gene therapy.

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Section: Inhibition Of Cell-associated Proteolysismentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Adenovirus-mediated delivery of a uPA/uPAR antagonist suppresses angiogenesis-dependent tumor growth and dissemination in mice

et al. 1998

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“…Apart from specifically displacing urokinase from its cell surface receptor, the hybrid molecule could also inhibit pro-urokinase-dependent plasminogen activation in the presence of u-PAR-bearing cells as well as in vitro tumor cell invasiveness [15]. In this study, we addressed the effect of the blockage of u-PAR by ATF-HSA or anti-u-PAR antibodies on the migration of endothelial cells and compared its effect with that of aprotinin, a potent inhibitor of plasmin.…”

Section: Introductionmentioning

confidence: 99%

Blockage of urokinase receptor reduces in vitro the motility and the deformability of endothelial cells

Lű

Mabilat

Yeh³

et al. 1996

FEBS Letters

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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 potent than plasmin inhibitors, suggesting that it exerts its effects not solely by inhibiting the remodeling of the extracellular matrix. In fact, analysis of the cell shape change during migration revealed for the first time that its effect is related to a decrease in cell deformability. These results suggest that u-PAR antagonist may be a new approach to control angiogenesis.

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“…A fusion protein harboring the amino-terminal part of uPA (aa 1Ϫ135) and human serum albumin (ATF-HSA hybrid) significantly reduced the invasive capacity of a breast cancer cell line in vitro (27). Similarly, a uPA-(1-137)/IgG chimera suppressed the metastatic capacity of human PC3 prostate carcinoma cells in nude mice (28).…”

Section: Discussionmentioning

confidence: 99%

“…Hybrid molecules harboring different parts of the two serpins, ␣ 1 -proteinase inhibitor and thyroxine-binding globulin, inhibited human leukocyte elastase and bound to thyroxine with high affinity (31). Nevertheless, all of the chimeric proteins discussed here have been constructed by fusion of independent domains of different proteins (27,30,(32)(33)(34) or by fusion of modules of structurally highly conserved proteins based on their modular architecture (31). In contrast, the presented cystatin variants have been generated, in a novel approach, by replacing 11 aa of the parent cystatin sequence with 13 aa of uPA, resulting in a biologically bifunctional active protein.…”

Section: Discussionmentioning

confidence: 99%

A Novel Type of Bifunctional Inhibitor Directed against Proteolytic Activity and Receptor/Ligand Interaction

Muehlenweg¹,

Assfalg-Machleidt²,

Parrado³

et al. 2000

Journal of Biological Chemistry

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Cancer invasion and metastasis is a process requiring a coordinated series of (anti-)adhesive, migratory, and pericellular proteolytic events involving various proteases such as urokinase-type plasminogen activator (uPA)/plasmin, cathepsins B and L, and matrix metalloproteases. Novel types of double-headed inhibitors directed to different tumor-associated proteolytic systems were generated by substitution of a loop in chicken cystatin, which is nonessential for cysteine protease inhibition, with uPA-derived peptides covering the human uPA receptor binding sequence uPA-

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Blockage of the urokinase receptor on the cell surface: Construction and characterization of a hybrid protein consisting of the N‐terminal fragment of human urokinase and human albumin

Cited by 34 publications

References 24 publications

Adenovirus-mediated delivery of a uPA/uPAR antagonist suppresses angiogenesis-dependent tumor growth and dissemination in mice

Adenovirus-mediated delivery of a uPA/uPAR antagonist suppresses angiogenesis-dependent tumor growth and dissemination in mice

Blockage of urokinase receptor reduces in vitro the motility and the deformability of endothelial cells

A Novel Type of Bifunctional Inhibitor Directed against Proteolytic Activity and Receptor/Ligand Interaction

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