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通过同种异型细胞粘附聚糖的单分子力谱研究蛋白聚糖力学。

Proteoglycan mechanics studied by single-molecule force spectroscopy of allotypic cell adhesion glycans.

作者信息

Garcia-Manyes Sergi, Bucior Iwona, Ros Robert, Anselmetti Dario, Sanz Fausto, Burger Max M, Fernàndez-Busquets Xavier

机构信息

Research Center for Bioelectronics and Nanobioscience, Barcelona Science Park, University of Barcelona, Josep Samitier 1-5, Barcelona E-08028, Spain.

出版信息

J Biol Chem. 2006 Mar 3;281(9):5992-9. doi: 10.1074/jbc.M507878200. Epub 2005 Dec 22.

Abstract

Early Metazoans had to evolve the first cell adhesion system addressed to maintaining stable interactions between cells constituting different individuals. As the oldest extant multicellular animals, sponges are good candidates to have remnants of the molecules responsible for that crucial innovation. Sponge cells associate in a species-specific process through multivalent calcium-dependent interactions of carbohydrate structures on an extracellular membrane-bound proteoglycan termed aggregation factor. Single-molecule force spectroscopy studies of the mechanics of aggregation factor self-binding indicate the existence of intermolecular carbohydrate adhesion domains. A 200-kDa aggregation factor glycan (g200) involved in cell adhesion exhibits interindividual differences in size and epitope content which suggest the existence of allelic variants. We have purified two of these g200 distinct forms from two individuals of the same sponge species. Comparison of allotypic versus isotypic g200 binding forces reveals significant differences. Surface plasmon resonance measurements show that g200 self-adhesion is much stronger than its binding to other unrelated glycans such as chondroitin sulfate. This adhesive specificity through multiple carbohydrate binding domains is a type of cooperative interaction that can contribute to explain some functions of modular proteoglycans in general. From our results it can be deduced that the binding strength/surface area between two aggregation factor molecules is comparable with that of focal contacts in vertebrate cells, indicating that strong carbohydrate-based cell adhesions evolved at the very start of Metazoan history.

摘要

早期后生动物必须进化出首个细胞黏附系统,以维持构成不同个体的细胞之间的稳定相互作用。作为现存最古老的多细胞动物,海绵很可能保留着负责这一关键创新的分子遗迹。海绵细胞通过一种细胞外膜结合蛋白聚糖(称为聚集因子)上碳水化合物结构的多价钙依赖性相互作用,以物种特异性的方式相互结合。对聚集因子自结合机制的单分子力谱研究表明存在分子间碳水化合物黏附结构域。参与细胞黏附的一种200 kDa聚集因子聚糖(g200)在大小和表位含量上存在个体间差异,这表明存在等位基因变体。我们从同一种海绵的两个个体中纯化出了两种不同形式的g200。对同种异型与同型g200结合力的比较揭示了显著差异。表面等离子体共振测量表明,g200的自黏附力远强于其与其他不相关聚糖(如硫酸软骨素)的结合力。这种通过多个碳水化合物结合结构域实现的黏附特异性是一种合作相互作用,总体上有助于解释模块化蛋白聚糖的一些功能。从我们的结果可以推断,两个聚集因子分子之间的结合强度/表面积与脊椎动物细胞中的黏着斑相当,这表明基于碳水化合物的强细胞黏附在动物历史的最初阶段就已进化出来。

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