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Activated platelets provide a functional microenvironment for the antiangiogenic fragment of histidine-rich glycoprotein.

Molecular cancer research : MCR (2009-11-12)
Asa Thulin, Maria Ringvall, Anna Dimberg, Karin Kårehed, Timo Väisänen, Marja-Riitta Väisänen, Osama Hamad, Jian Wang, Rolf Bjerkvig, Bo Nilsson, Taina Pihlajaniemi, Helena Akerud, Kristian Pietras, Wilhelm Jahnen-Dechent, Agneta Siegbahn, Anna-Karin Olsson
RÉSUMÉ

The angiogenesis inhibitor histidine-rich glycoprotein (HRG) constitutes one of several examples of molecules regulating both angiogenesis and hemostasis. The antiangiogenic properties of HRG are mediated via its proteolytically released histidine- and proline-rich (His/Pro-rich) domain. Using a combination of immunohistochemistry and mass spectrometry, we here provide biochemical evidence for the presence of a proteolytic peptide, corresponding to the antiangiogenic domain of HRG, in vivo in human tissue. This finding supports a role for HRG as an endogenous regulator of angiogenesis. Interestingly, the His/Pro-rich peptide bound to the vessel wall in tissue from cancer patients but not to the vasculature in tissue from healthy persons. Moreover, the His/Pro-rich peptide was found in close association with platelets. Relesate from in vitro-activated platelets promoted binding of the His/Pro-rich domain of HRG to endothelial cells, an effect mediated by Zn(2+). Previous studies have shown that zinc-dependent binding of the His/Pro-rich domain of HRG to heparan sulfate on endothelial cells is required for inhibition of angiogenesis. We describe a novel mechanism to increase the local concentration and activity of an angiogenesis inhibitor, which may reflect a host response to counteract angiogenesis during pathologic conditions. Our finding that tumor angiogenesis is elevated in HRG-deficient mice supports this conclusion.

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Anti-Vitronectin Antibody, clone BV2, clone BV2, Chemicon®, from mouse