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首页> 外文期刊>Acta biomaterialia >Interactions of the streptococcal C5a peptidase with human fibronectin.
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Interactions of the streptococcal C5a peptidase with human fibronectin.

机译:链球菌C5a肽酶与人纤连蛋白的相互作用。

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摘要

Group B Streptococci (GBS) is a leading cause of sepsis and meningitis in neonates and immunocompromised adults in western countries. GBS do not bind to fibronectin (Fn) in solution, but will bind to Fn adsorbed onto a solid surface. The reason for the specificity of this binding is unknown. Single molecule force spectroscopy was used to test the hypothesis that GBS, through streptococcal C5a peptidase (ScpB) molecules present on the surface of the bacteria, binds to a motif created by the juxtaposition of multiple adjacent Fn molecules. Atomic force microscopy (AFM) topographical images of adsorbed Fn deposited from various Fn coating concentrations were used to determine the Fn surface concentration. ScpB was tethered to an AFM tip with all surface modifications characterized by X-ray photoelectron spectroscopy and time-of-flight secondary ion mass spectrometry. At the lowest Fn coverages the probability of observing a ScpB-Fn binding event increased linearly with Fn surface coverage. As an Fn monolayer was reached the probability of a ScpB-Fn binding event occurring increased markedly ( approximately 50 fold), with a concomitant increase in the rupture force from 17 pN to 33 pN. These results are consistent with the hypothesis that ScpB binds to a motif created by the juxtaposition of multiple Fn molecules.
机译:B组链球菌(GBS)是西方国家新生儿和免疫功能低下的成年人败血症和脑膜炎的主要原因。 GBS在溶液中不与纤连蛋白(Fn)结合,但会与吸附到固体表面的Fn结合。这种结合的特异性的原因是未知的。单分子力谱法用于检验以下假设:GBS通过细菌表面上存在的链球菌C5a肽酶(ScpB)分子与多个相邻Fn分子并列产生的基序结合。从各种Fn涂层浓度沉积的吸附Fn的原子力显微镜(AFM)地形图用于确定Fn表面浓度。 ScpB被束缚到AFM尖端,其所有表面修饰均以X射线光电子能谱和飞行时间二次离子质谱为特征。在最低的Fn覆盖率下,观察到ScpB-Fn结合事件的概率随Fn表面覆盖率线性增加。当达到Fn单层时,发生ScpB-Fn结合事件的可能性显着增加(大约50倍),同时断裂力也从17 pN增加到33 pN。这些结果与ScpB结合由多个Fn分子并置产生的基序的假说相符。

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