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The effects of streptavidin-biotin exogenous ligands on the endothelium-derived nitric oxide synthase activity

机译:链霉亲和素-生物素外源配体对内皮源性一氧化氮合酶活性的影响

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In this study, the effects of the streptavidin (SA)-biotin ligands on the amount of endothelium-derived nitric oxide synthase (eNOS) were quantified. The higher-affinity SA-biotin ligands were previously introduced to help promote the initial endothelial cell attachment to fibronectin coated surfaces. To validate their applications, SA-biotin ligands must be demonstrated to have minimal adverse effects on the eNOS activity, a process that is crucial to the vasotone regulation. Results in this study suggest that not only did the SA-biotin ligands have no adverse effects on the eNOS activity, they significantly promoted it. We speculate that this experimental observation is likely due to the enhancement of the different cell adhesion parameters, including the cellular spreading, cell adhesion strength, as well as the formation of focal contacts. Because of the improvement of these parameters, the cells were able to attach onto the surfaces more rapidly and firmly, thereby enabling the formation of a stable and rapidly crosslinked cell cytoskeletal network. The development and formation of such stable cytoskeleton is crucial for the shear stress signals to transmit through the cell and to eventually activate the different intracellular events that are required to promote the eNOS activity.
机译:在这项研究中,对链霉亲和素(SA)-生物素配体对内皮源性一氧化氮合酶(eNOS)数量的影响进行了定量。先前引入了较高亲和力的SA-生物素配体,以帮助促进内皮细胞最初附着于纤连蛋白包被的表面。为了验证其应用,必须证明SA-生物素配体对eNOS活性具有最小的不利影响,而eNOS活性对血管紧张素的调节至关重要。这项研究的结果表明,SA-生物素配体不仅对eNOS活性没有不利影响,而且还显着促进了eNOS活性。我们推测该实验观察可能是由于不同细胞粘附参数的增强,包括细胞扩散,细胞粘附强度以及焦点接触的形成。由于这些参数的改善,细胞能够更快速和牢固地附着在表面上,从而能够形成稳定且快速交联的细胞细胞骨架网络。这种稳定的细胞骨架的形成和形成对于剪切应力信号通过细胞传递并最终激活促进eNOS活性所需的不同细胞内事件至关重要。

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