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(精氨酸-甘氨酸-天冬氨酸)n-白蛋白缀合物作为整合素介导细胞黏附的模型基质。

(Arg-Gly-Asp)n-albumin conjugates as a model substratum for integrin-mediated cell adhesion.

作者信息

Danilov Y N, Juliano R L

机构信息

Department of Pharmacology, School of Medicine, University of North Carolina, Chapel Hill 27599-7365.

出版信息

Exp Cell Res. 1989 May;182(1):186-96. doi: 10.1016/0014-4827(89)90290-5.

Abstract

We have prepared protein-peptide conjugates composed of bovine serum albumin (BSA) derivatized with short peptides containing the Arg-Gly-Asp (RGD) sequence derived from the adhesion site of fibronectin. The RGD-BSA conjugates were used to coat tissue culture plastic surfaces which then served as substrata in cell adhesion experiments. Our results indicate that the efficiency of adhesion to RGD-BSA-coated surfaces is highly dependent on the valency of the (RGD)n-BSA conjugates. For example, on surfaces with approximately equal amounts of RGD ligand, CHO cells adhered virtually 100% to the (RGD)n-BSA (n = 20.8) conjugate and not at all to the (RGD)n-BSA (n = 3.5) conjugate. Adhesion on (RGD)n-BSA-coated substrata and on fibronectin- or vitronectin-coated substrata was also examined in terms of the relationship between cell adhesion and the intermolecular distances of adsorbed proteins. It was observed that for substrata coated with relatively compact, symmetric molecules, such as RGD-BSA or vitronectin, adhesion dropped off sharply as intermolecular distances increased; by contrast, for fibronectin, a large asymmetric molecule, adhesion declined more gradually as intermolecular distances increased. Finally, we have examined the role of different cell-surface receptors in the process of adhesion to RGD-BSA substrata. Interestingly, competition and blocking experiments with antibodies and with soluble competing proteins suggest that it is the vitronectin receptor rather than the fibronectin receptor which mediates adhesion to RGD-BSA.

摘要

我们制备了蛋白质 - 肽缀合物,其由牛血清白蛋白(BSA)与源自纤连蛋白粘附位点的含精氨酸 - 甘氨酸 - 天冬氨酸(RGD)序列的短肽衍生化而成。RGD - BSA缀合物用于包被组织培养塑料表面,然后在细胞粘附实验中用作底物。我们的结果表明,对RGD - BSA包被表面的粘附效率高度依赖于(RGD)n - BSA缀合物的价态。例如,在具有大致等量RGD配体的表面上,CHO细胞几乎100%粘附于(RGD)n - BSA(n = 20.8)缀合物,而完全不粘附于(RGD)n - BSA(n = 3.5)缀合物。还根据细胞粘附与吸附蛋白分子间距离之间的关系,研究了在(RGD)n - BSA包被的底物以及纤连蛋白或玻连蛋白包被的底物上的粘附情况。观察到,对于用相对紧密、对称的分子如RGD - BSA或玻连蛋白包被的底物,随着分子间距离增加,粘附急剧下降;相比之下,对于大的不对称分子纤连蛋白,随着分子间距离增加,粘附下降更为缓慢。最后,我们研究了不同细胞表面受体在粘附到RGD - BSA底物过程中的作用。有趣的是,用抗体和可溶性竞争蛋白进行的竞争和阻断实验表明,介导对RGD - BSA粘附的是玻连蛋白受体而非纤连蛋白受体。

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