首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Forced unfolding of the fibronectin type III module reveals a tensile molecular recognition switch
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Forced unfolding of the fibronectin type III module reveals a tensile molecular recognition switch

机译:强制展开纤连蛋白III型模块揭示了拉伸分子识别开关

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摘要

The 10th type III module of fibronectin pos- sesses a beta-sandwich structure consisting of seven beta-strands (AG) that are arranged in two antiparallel sheets. It mediates cell adhesion to surfaces via its integrin binding motif, Arg78, GIy79, and Asp80 (RGD), which is placed at the apex of the loop connecting beta-strands F and G. Stecred molecular dynamics simulations in which tension is applied to the protein's terminal ends reveal that the beta-strand G is the first to break away from the module on forced unfolding whereas the remaining fold maintains its structural integrity. The sepa- ration of strand G from the remaining fold results in a gradual shortening of the distance between the apex of the RGD- containing loop and the module surface, which potentially reduces the loop's accessibility to surface-bound integrins. The shortening is followed by a straightening of the RGD-loop from a tight beta-turn into a linear conformation, which suggests a further decrease of affinity and selectivity to integrins. The RGD-loop therefore is located strategically to undergo strong conformational changes in the early stretching stages of the module and thus constitutes a mechanosensitive control of ligand recognition.
机译:纤连蛋白的第10类III型模块具有β三明治结构,该结构由7个β链(AG)组成,并排列在两个反平行的薄片中。它通过整合素结合基序Arg78,Gly79和Asp80(RGD)介导细胞对表面的粘附,后者位于连接β链F和G的环的顶点。Stecred分子动力学模拟,其中张力施加于蛋白质的末端显示,β链G在强制展开时是第一个脱离模块的,而其余的折叠则保持了其结构完整性。链G与其余折叠的分离导致含RGD的环的顶点与模块表面之间的距离逐渐缩短,从而潜在地降低了环对表面结合的整联蛋白的可及性。缩短之后,RGD环从紧密的β角转为线性构象,从而变直,这表明对整联蛋白的亲和力和选择性进一步降低。因此,RGD-环的位置具有战略意义,可以在模块的早期拉伸阶段经历强烈的构象变化,从而构成配体识别的机械敏感控制。

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