Literature DB >> 23709605

Domain 2 of uPAR regulates single-chain urokinase-mediated angiogenesis through β1-integrin and VEGFR2.

Gretchen A Larusch1, Alona Merkulova, Fakhri Mahdi, Zia Shariat-Madar, Robert G Sitrin, Douglas B Cines, Alvin H Schmaier.   

Abstract

How single-chain urokinase (ScuPA) mediates angiogenesis is incompletely understood. ScuPA (≥4 nM) induces phosphorylated (p)ERK1/2 (MAPK44 and MAPK42) and pAkt (Ser(473)) in umbilical vein and dermal microvascular endothelial cells. Activation of pERK1/2 by ScuPA is blocked by PD-98059 or U-0126, and pAkt (Ser(473)) activation is inhibited by wortmannin or LY-294002. ScuPA (32 nM) or protease-inhibited two-chain urokinase stimulates pERK1/2 to the same extent, indicating that signaling is not dependent on enzymatic activity. ScuPA induces pERK1/2, but not pAkt (Ser(473)), in SIN1(-/-) cells, indicating that the two pathways are not identical. Peptides from domain 2 of the urokinase plasminogen activator receptor (uPAR) or domain 5 of high-molecular-weight kininogen compete with ScuPA for the induction of pERK1/2 and pAkt (Ser(473)). A peptide of the integrin-binding site on uPAR, a β1-integrin peptide that binds uPAR, antibody 6S6 to β1-integrin, tyrosine kinase inhibitors AG-1478 or PP3, and small interfering RNA knockdown of VEFG receptor 2, but not HER1-HER4, blocked ScuPA-induced pERK1/2 and pAkt (Ser(473)). ScuPA-induced endothelial cell proliferation was blocked by inhibitors of pERK1/2 and pAkt (Ser(473)), antibody 6S6, and uPAR or kininogen peptides. ScuPA initiated aortic sprouts and Matrigel plug angiogenesis in normal, but not uPAR-deficient, mouse aortae or mice, respectively, but these were blocked by PD-98059, LY-294002, AG-1478, or cleaved high-molecular-weight kininogen. In summary, this investigation indicates a novel, a nonproteolytic signaling pathway initiated by zymogen ScuPA and mediated by domain 2 of uPAR, β1-integrins, and VEGF receptor 2 leading to angiogenesis. Kininogens or peptides from it downregulate this pathway.

Entities:  

Keywords:  epidermal growth factor receptors; high-molecular-weight kininogen; single-chain urokinase; urokinase plasminogen activator receptor; vascular epidermal growth factor receptor 2

Mesh:

Substances:

Year:  2013        PMID: 23709605      PMCID: PMC3742872          DOI: 10.1152/ajpheart.00110.2013

Source DB:  PubMed          Journal:  Am J Physiol Heart Circ Physiol        ISSN: 0363-6135            Impact factor:   4.733


  71 in total

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5.  Domain 2 of the urokinase receptor contains an integrin-interacting epitope with intrinsic signaling activity: generation of a new integrin inhibitor.

Authors:  Bernard Degryse; Massimo Resnati; Ralf-Peter Czekay; David J Loskutoff; Francesco Blasi
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Authors:  Yuchuan Liu; Irma M Sainz; Yi Wu; Robin Pixley; Ricardo G Espinola; Sarmina Hassan; Mohammad M Khan; Robert W Colman
Journal:  Exp Cell Res       Date:  2007-10-18       Impact factor: 3.905

9.  Plasmin-induced migration of endothelial cells. A potential target for the anti-angiogenic action of angiostatin.

Authors:  Takehiko Tarui; Mousumi Majumdar; Lindsey A Miles; Wolfram Ruf; Yoshikazu Takada
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10.  Urokinase-type plasminogen activator receptor is involved in mediating the apoptotic effect of cleaved high molecular weight kininogen in human endothelial cells.

Authors:  Dian J Cao; Yan-Lin Guo; Robert W Colman
Journal:  Circ Res       Date:  2004-03-25       Impact factor: 17.367

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2.  Urokinase-type Plasminogen Activator (uPA) Promotes Angiogenesis by Attenuating Proline-rich Homeodomain Protein (PRH) Transcription Factor Activity and De-repressing Vascular Endothelial Growth Factor (VEGF) Receptor Expression.

Authors:  Victoria Stepanova; Padma-Sheela Jayaraman; Sergei V Zaitsev; Tatiana Lebedeva; Khalil Bdeir; Rachael Kershaw; Kelci R Holman; Yelena V Parfyonova; Ekaterina V Semina; Irina B Beloglazova; Vsevolod A Tkachuk; Douglas B Cines
Journal:  J Biol Chem       Date:  2016-05-04       Impact factor: 5.157

3.  Vascular Endothelial Cells Produce Coagulation Factors That Control Their Growth via Joint Protease-Activated Receptor and C5a Receptor 1 (CD88) Signaling.

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4.  EGFR/uPAR interaction as druggable target to overcome vemurafenib acquired resistance in melanoma cells.

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Journal:  EBioMedicine       Date:  2019-01-02       Impact factor: 8.143

Review 5.  The uPAR System as a Potential Therapeutic Target in the Diseased Eye.

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6.  Construction and Verification of a Combined Hypoxia and Immune Index for Clear Cell Renal Cell Carcinoma.

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