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Determination of the association constant between the B domain of protein A and the Fc region of IgG

机译:确定蛋白A的B结构域与IgG的Fc区之间的缔合常数

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摘要

The aim of this work is the numerical modelling of the binding mechanism between the Fc region of human IgG interacting with the B domain of Staphylococcal protein A (SpA). The comprehension of the involved kinetics is of noticeable impact for immunosensor diagnostic applications and consequently contributes to increase the sensitivity and efficiency of such devices based on the immobilization of antibodies on biosensor surface. Brownian dynamics methodology is applied to simulate the Fc-SpA encounter. Then, the association rates k_(on) and k_(off) are estimated from the analysis of the diffusional motion between the Fc region and the B domain of SpA combined with continuum electrostatic calculations. Therefore, the association constant K_a between Fc and SpA is calculated. The behaviour of K_a is analysed taking into account the relative distance between SpA and the Fc fragments. The analyses also include the effects on the binding affinity between SpA and Fc due to the variation of the solvent ionic strength and pH values. The association rates and their analyses are presented and discussed showing that the binding mechanism between the SpA and the Fc fragments is enhanced by the nonpolar interaction, while dissociation is driven by the electrostatic repulsion that occurs at relatively low pH. The numerical estimation of the association constant will support the definition of robust protocols for the detection of antibodies via protein A.
机译:这项工作的目的是对人IgG的Fc区与葡萄球菌蛋白A(SpA)的B结构域相互作用的结合机制进行数值模拟。所涉及的动力学的理解对于免疫传感器诊断应用具有显着影响,因此基于抗体在生物传感器表面上的固定化而有助于提高此类设备的灵敏度和效率。布朗动力学方法学被用于模拟Fc-SpA遭遇。然后,结合连续电学静电计算,通过分析SpA的Fc区和B结构域之间的扩散运动来估计缔合率k_(on)和k_(off)。因此,计算出Fc与SpA之间的缔合常数K_a。考虑到SpA和Fc片段之间的相对距离来分析K_a的行为。分析还包括由于溶剂离子强度和pH值的变化而对SpA和Fc之间的结合亲和力的影响。提出并讨论了缔合速率及其分析,结果表明SpA与Fc片段之间的结合机制通过非极性相互作用得到增强,而离解是通过在相对较低pH值下发生的静电排斥来驱动的。关联常数的数值估计将支持定义可靠的方案以通过蛋白A检测抗体。

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