Urokinase plasminogen activator receptor, beta 2-integrins, and Src-kinases within a single receptor complex of human monocytes.
10.1084/jem.181.4.1381
Crossref journal-article
Rockefeller University Press
The Journal of experimental medicine (291)
Abstract

The glycosylphosphatidylinositol (GPI)-anchored membrane protein urokinase plasminogen activator-receptor (uPA-R; CD87) is one of the key molecules involved in migration of leukocytes and tumor cells. uPA bound to uPA-R provides the cell proteolytic potential used for degradation of extracellular matrix. uPA-R is also involved in induction of cell adhesion and chemotaxis. Here, we provide a molecular explanation for these uPA-R-related cellular events. By size fractionation of monocyte lysate and affinity isolation on its natural ligand uPA, we demonstrate uPA-R as a component of a receptor complex of relatively large size. Reprecipitation and immunoblotting techniques allowed us to detect the protein tyrosine kinases (PTKs) p60fyn, p53/56lyn, p58/64hck, and p59fgr as components of this "uPA-R complex". Activation of monocytes even with enzymatically inactivated uPA resulted in induction of tyrosine phosphorylation, suggesting modulation of uPA-R-associated PTKs upon ligand binding. In spite of their presence in large complexes, we did not find the GPI-linked proteins CD14, CD58, and CD59 in the uPA-R complex, which indicates the presence of different receptor domains containing GPI-linked proteins in monocytes. However, we identified the leukocyte integrins LFA-1 and CR3 as components of the uPA-R complex as indicated by coisolation of these molecules, as well as by cocapping and comodulation of uPA-R and leukocyte integrins on the monocyte surface. The assemblage of uPA-R, PTKs and membrane spanning beta 2-integrins in one receptor complex indicates functional cooperation. In regard to the involvement of these molecules in pericellular proteolysis, signal transduction, as well as adhesion and chemotactic movement, we suggest uPA-R complex as a potential cellular device for cell migration.

Bibliography

Bohuslav, J., Horejsí, V., Hansmann, C., Stöckl, J., Weidle, U. H., Majdic, O., Bartke, I., Knapp, W., & Stockinger, H. (1995). Urokinase plasminogen activator receptor, beta 2-integrins, and Src-kinases within a single receptor complex of human monocytes. The Journal of Experimental Medicine, 181(4), 1381–1390.

Authors 9
  1. J Bohuslav (first)
  2. V Horejsí (additional)
  3. C Hansmann (additional)
  4. J Stöckl (additional)
  5. U H Weidle (additional)
  6. O Majdic (additional)
  7. I Bartke (additional)
  8. W Knapp (additional)
  9. H Stockinger (additional)
References 0 Referenced 269

None

Dates
Type When
Created 21 years, 2 months ago (June 24, 2004, 3:56 a.m.)
Deposited 2 years, 1 month ago (July 25, 2023, 2:42 a.m.)
Indexed 2 weeks, 6 days ago (Aug. 7, 2025, 4:53 a.m.)
Issued 30 years, 4 months ago (April 1, 1995)
Published 30 years, 4 months ago (April 1, 1995)
Published Online 30 years, 4 months ago (April 1, 1995)
Published Print 30 years, 4 months ago (April 1, 1995)
Funders 0

None

@article{Bohuslav_1995, title={Urokinase plasminogen activator receptor, beta 2-integrins, and Src-kinases within a single receptor complex of human monocytes.}, volume={181}, ISSN={1540-9538}, url={http://dx.doi.org/10.1084/jem.181.4.1381}, DOI={10.1084/jem.181.4.1381}, number={4}, journal={The Journal of experimental medicine}, publisher={Rockefeller University Press}, author={Bohuslav, J and Horejsí, V and Hansmann, C and Stöckl, J and Weidle, U H and Majdic, O and Bartke, I and Knapp, W and Stockinger, H}, year={1995}, month=apr, pages={1381–1390} }