Cao Dian J, Guo Yan-Lin, Colman Robert W
Sol Sherry Thrombosis Research Center, Temple University School of Medicine, Philadelphia, Pa 19140, USA.
Circ Res. 2004 May 14;94(9):1227-34. doi: 10.1161/01.RES.0000126567.75232.46. Epub 2004 Mar 25.
Cleaved high molecular weight kininogen (HKa) has been shown to inhibit in vivo neovascularization and induce apoptosis of endothelial cells. We have shown that HKa-induced apoptosis correlated with its antiadhesive effect and was regulated by extracellular matrix (ECM) proteins. In this study, we identified the urokinase-type plasminogen activator receptor (uPAR) as a target of HKa activity at the endothelial cell surface. Anti-uPAR antibodies blocked the apoptotic effect of HKa. Further studies revealed that uPAR formed a signaling complex containing integrin alpha(v)beta3 or alpha5beta1, caveolin, and Src kinase Yes in endothelial cells. HKa physically disrupted the formation of this complex in a manner that paralleled its apoptotic effect. For the first time, our results provide a mechanistic explanation for the previous observation that HKa selectively induces apoptosis of endothelial cells grown on vitronectin, but not cells grown on fibronectin. These data also resolve the controversial role of uPAR in mediating the apoptotic and antiadhesive activities of HKa.
裂解的高分子量激肽原(HKa)已被证明可抑制体内新血管形成并诱导内皮细胞凋亡。我们已经表明,HKa诱导的凋亡与其抗黏附作用相关,并受细胞外基质(ECM)蛋白调节。在本研究中,我们确定尿激酶型纤溶酶原激活物受体(uPAR)是HKa在内皮细胞表面的活性靶点。抗uPAR抗体可阻断HKa的凋亡作用。进一步研究表明,uPAR在内皮细胞中形成了一个包含整合素α(v)β3或α5β1、小窝蛋白和Src激酶Yes的信号复合物。HKa以与其凋亡作用平行的方式物理性破坏了该复合物的形成。我们的结果首次为之前的观察结果提供了一个机制解释,即HKa选择性诱导在玻连蛋白上生长的内皮细胞凋亡,但不诱导在纤连蛋白上生长的细胞凋亡。这些数据也解决了uPAR在介导HKa的凋亡和抗黏附活性方面的争议性作用。
