Thrombin promotes endothelial cell alignment in Matrigel in vitro and angiogenesis in vivo
G. C. Haralabopoulos, D. S. Grant, H. K. Kleinman and M. E. Maragoudakis Department of Pharmacology, University of Patras Medical School, Greece. We have tested the effect of thrombin on endothelial cell tube formation in vitro and angiogenesis in vivo. Thrombin induces the differentiation of endoth...
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Veröffentlicht in: | American Journal of Physiology: Cell Physiology 1997-07, Vol.273 (1), p.C239-C245 |
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Zusammenfassung: | G. C. Haralabopoulos, D. S. Grant, H. K. Kleinman and M. E. Maragoudakis
Department of Pharmacology, University of Patras Medical School, Greece.
We have tested the effect of thrombin on endothelial cell tube formation in
vitro and angiogenesis in vivo. Thrombin induces the differentiation of
endothelial cells into capillary structures in a dose-dependent fashion
(0.1-0.3 units thrombin/ml) on Matrigel, a laminin-rich reconstituted
basement membrane matrix. At higher thrombin concentrations (1.0 unit/ml),
a suppression of tube formation is evident, probably due to downregulation
(desensitization) of the thrombin receptor. D-Phe-Pro-Arg-CH2Cl-thrombin is
without effect when used alone, but it abolishes the tube-promoting effect
of thrombin when used in combination with thrombin, indicating the
involvement of the catalytic site of thrombin. Activation of protein kinase
C (PKC) seems to be the transduction mechanism involved in the stimulation
of tube formation by thrombin. Ro-318220 (3 micrograms/ml), a specific
inhibitor of PKC, completely abolishes the stimulatory effect of thrombin.
In the in vivo Matrigel system of angiogenesis, there is a 10-fold increase
in endothelial cell infiltration in response to thrombin. These results
provide evidence for the angiogenesis-promoting effect of thrombin in vivo
and the induction by thrombin of the angiogenic phenotype of endothelial
cells in vitro in the absence of other cell types such as smooth muscle
cells, pericytes, and inflammatory cells. |
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ISSN: | 0363-6143 0002-9513 1522-1563 2163-5773 |
DOI: | 10.1152/ajpcell.1997.273.1.c239 |