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Surface plasmon fluorescence measurements of human chorionic gonadotrophin: Role of antibody orientation in obtaining enhanced sensitivity and limit of detection

机译:人绒毛膜促性腺激素的表面等离激元荧光测量:抗体定向在获得增强的灵敏度和检测限中的作用

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This paper describes the determination of limits of detection (LODs) of interactions between an antigen, human chorionic gonadotrophin (hCG), and antibodies, anti-alpha-hCG and anti-beta-hCG, using a sandwich assay by surface plasmon field-enhanced fluorescence spectroscopy (SPFS). Randomly biotinylated antibodies were adsorbed onto a structured self-assembled monolayer (SAM)-streptavidin matrix, tethered to gold via a SAM consisting of biotinylated thiol molecules interspersed with hydroxyalkanethiol molecules. The influence of the concentration of biotinylated thiol on the binding of biotinylated antibody and its functionality, in terms of its ability to bind to the hCG antigen, was studied. This allowed determination of the optimum biotin-thiol mole fraction in the mixed thiol solution and consequently in the SAM, to maximize binding of hCG of the streptavidin-bound antibody. SPFS studies of the binding of a secondary fluorescently labeled antibody to hCG immobilized on the optimized SAM-streptavidin-antibody layer showed that a LOD of hCG of 2 mIU mL(-1) (4 x 10(-12) mol L-1) could be realized. The system was further optimized by using a more oriented and organized surface by adsorbing monobiotinylated Fab-hCG in place of the whole antibody. A LOD of 0.3 mIU mL(-1) (6 x 10(-13) mol L-1) was achieved for this system. This work illustrates the importance of antibody orientation, both on the planar surface and in terms of position of binding site, in maximizing sensor sensitivity.
机译:本文介绍了通过表面等离子体激元场增强的三明治测定法确定抗原,人绒毛膜促性腺激素(hCG)与抗体,抗α-hCG和抗β-hCG之间相互作用的检测限(LOD)荧光光谱(SPFS)。随机将生物素化抗体吸附到结构化的自组装单层(SAM)-链霉亲和素基质上,并通过由生物素化硫醇分子和羟基链烷硫醇分子组成的SAM束缚在金上。研究了生物素化硫醇的浓度对生物素化抗体结合及其功能的影响,就其与hCG抗原的结合能力而言。这使得可以确定混合硫醇溶液中以及随后在SAM中的最佳生物素-硫醇摩尔分数,以最大化链霉亲和素结合抗体的hCG结合。 SPFS研究第二荧光标记抗体与固定在优化SAM-链霉亲和素抗体层上的hCG的结合表明,hCG的LOD为2 mIU mL(-1)(4 x 10(-12)mol L-1)可以实现。通过吸附单生物素化的Fab-hCG代替整个抗体,使用更加定向和组织化的表面,进一步优化了系统。此系统的LOD为0.3 mIU mL(-1)(6 x 10(-13)mol L-1)。这项工作说明了在平面上以及在结合位点位置方面,抗体定向在最大化传感器灵敏度方面的重要性。

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