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整合素β1和β3介导的内皮细胞迁移是通过不同的信号传导机制触发的。

Integrin beta 1- and beta 3-mediated endothelial cell migration is triggered through distinct signaling mechanisms.

作者信息

Leavesley D I, Schwartz M A, Rosenfeld M, Cheresh D A

机构信息

Department of Immunology, Scripps Research Institute, La Jolla, California 92037.

出版信息

J Cell Biol. 1993 Apr;121(1):163-70. doi: 10.1083/jcb.121.1.163.

Abstract

Human umbilical vein endothelial cell attachment, spreading and migration on collagen and vitronectin are mediated by integrins alpha 2 beta 1 and alpha v beta 3, respectively, and these events take place in the absence of cytokines, growth factors, or chemoattractants. Cell attachment and spreading on these ligands occur in the absence of extracellular calcium, as does migration on collagen. In contrast, vitronectin-mediated migration is absolutely dependent on the presence of extracellular calcium. Cell contact with immobilized vitronectin or anti-alpha v beta 3 mAbs promotes a measurable rise in [Ca2+]i which requires an extracellular calcium source, whereas collagen, or anti-alpha 2 beta 1 mAbs fail to promote this signaling event. In fact, vitronectin-mediated migration and the rise in intracellular calcium showed the same dose dependence on extracellular calcium. While vitronectin and collagen differ in their ability to induce a calcium influx both ligands or antibodies to their respective integrins promote an equivalent increase in intracellular pH consistent with activation of the Na/H antiporter an event independent of extracellular calcium. These results support two salient conclusions. Firstly, collagen and vitronectin, through their respective integrins, promote distinct intracellular signaling events. Secondly, the alpha v beta 3 specific influx of calcium is not required for cell spreading yet appears to facilitate cellular migration on vitronectin.

摘要

人脐静脉内皮细胞在胶原蛋白和玻连蛋白上的黏附、铺展和迁移分别由整合素α2β1和αvβ3介导,并且这些过程在没有细胞因子、生长因子或趋化因子的情况下发生。细胞在这些配体上的黏附和铺展在没有细胞外钙的情况下发生,在胶原蛋白上的迁移也是如此。相比之下,玻连蛋白介导的迁移绝对依赖于细胞外钙的存在。细胞与固定化的玻连蛋白或抗αvβ3单克隆抗体接触会促进[Ca2+]i可测量的升高,这需要细胞外钙源,而胶原蛋白或抗α2β1单克隆抗体则无法促进这一信号事件。事实上,玻连蛋白介导的迁移和细胞内钙的升高对细胞外钙表现出相同的剂量依赖性。虽然玻连蛋白和胶原蛋白在诱导钙内流的能力上有所不同,但它们各自整合素的配体或抗体都会促进细胞内pH的同等升高,这与钠氢反向转运体的激活一致,这是一个独立于细胞外钙的事件。这些结果支持两个显著结论。首先,胶原蛋白和玻连蛋白通过各自的整合素促进不同的细胞内信号事件。其次,细胞铺展不需要αvβ3特异性的钙内流,但它似乎促进了细胞在玻连蛋白上的迁移。

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