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链霉亲和素RGD突变体对内皮细胞黏附的影响。

Effect of streptavidin RGD mutant on the adhesion of endothelial cells.

作者信息

Chan Bernard P, Reichert William M, Truskey George A

机构信息

Department of Biomedical Engineering, Duke University, Durham, North Carolina 27708-0281, USA.

出版信息

Biotechnol Prog. 2004 Mar-Apr;20(2):566-75. doi: 10.1021/bp034215z.

Abstract

Adhesion of endothelial cells (EC) to surfaces can be enhanced by supplementing the integrin-mediated adhesion with high-affinity streptavidin (SA) that links a biotinylated EC to a biotinylated surface. Biotin pullout from the EC membrane limits the effectiveness of this treatment, leading to a predominance of EC detachment by cohesive failure. In this study we investigated whether a RGD-SA mutant that links SA to EC integrin receptors, and eliminates EC biotinylation, improves EC adhesion. Suspended EC were incubated with the RGD-SA mutant prior to cell seeding, primarily via attachment to the RGD binding site on alpha(v)beta(3) integrin. RGD-SA-incubated EC were subsequently seeded onto a surface preadsorbed with a mixture of fibronectin (Fn) and biotinylated bovine serum albumin (b-BSA). Results showed EC adhesion supplemented with the RGD-SA-biotin system significantly increased cell retention under flow, critical shear stresses for detachment, focal contact area, and force per bond relative to SA used with biotinylated EC. These increases were accompanied by significant reductions in membrane fragments left behind following EC detachment, which suggested cohesive failure via cell membrane rupture was significantly reduced, and enhanced phosphorylation of focal adhesion kinase, which suggested activation and clustering of integrin receptors. Together, these results show that the integrin-independent augmentation of EC adhesion using SA-biotin can be further improved through use of an RGD-SA mutant.

摘要

通过用高亲和力链霉亲和素(SA)补充整合素介导的黏附作用,可增强内皮细胞(EC)与表面的黏附,SA能将生物素化的EC与生物素化的表面连接起来。从EC膜中拔出生物素会限制这种处理的效果,导致EC因内聚性破坏而大量脱离。在本研究中,我们调查了一种将SA与EC整合素受体相连并消除EC生物素化的RGD-SA突变体是否能改善EC黏附。在细胞接种前,将悬浮的EC与RGD-SA突变体孵育,主要是通过附着于α(v)β(3)整合素上的RGD结合位点。随后将经RGD-SA孵育的EC接种到预先吸附有纤连蛋白(Fn)和生物素化牛血清白蛋白(b-BSA)混合物的表面。结果显示,与用于生物素化EC的SA相比,补充了RGD-SA-生物素系统的EC黏附在流动条件下显著增加了细胞保留率、脱离的临界剪切应力、黏着斑面积和每个键的力。这些增加伴随着EC脱离后留下的膜碎片显著减少,这表明通过细胞膜破裂的内聚性破坏显著减少,同时黏着斑激酶的磷酸化增强,这表明整合素受体被激活并聚集。总之,这些结果表明,通过使用RGD-SA突变体,利用SA-生物素对EC黏附进行不依赖整合素的增强作用可得到进一步改善。

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