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基于“软着陆”抗体固定化机制的高性能免疫乳胶的研制。

Development of a high-performance immunolatex based on "soft landing" antibody immobilization mechanism.

机构信息

Department of Materials Sciences, Graduate School of Pure and Applied Sciences, University of Tsukuba, Tennodai 1-1-1, Tsukuba, Ibaraki 305-8573, Japan.

出版信息

Colloids Surf B Biointerfaces. 2012 Nov 1;99:45-52. doi: 10.1016/j.colsurfb.2011.09.040. Epub 2011 Sep 29.

Abstract

Rabbit anti-human ferritin (anti-hFT) polyclonal immunoglobulin G (IgG) and poly(ethylene glycol) (PEG) were sequentially co-immobilized onto polystyrene submicroparticles (sMPs) to construct sMP/anti-hFT/PEG (SAP) immunolatex. Chemical immobilization of anti-hFT was performed at different pH levels to evaluate variations in antigen recognition. Basic pH disfavored conjugation of anti-hFT to sMPs, but remarkably increased its antigen recognition in comparison to that at neutral pH. We investigated this intriguing phenomenon further by assessing the kinetics of antibody binding, including the time-dependency of immobilization, antigen recognition, and orientation of bound anti-hFT. Therefore, we attributed high antigen recognition to significant electrostatic repulsion between sMPs and anti-hFT at basic pH, which predominately prevented anti-hFT access to sMPs and concurrently promoted anti-hFT orientations suitable for antigen recognition. Subsequent PEG modification maintained such anti-hFT orientation, without which antigen-accessible orientations would have decreased with time. Thus, properly oriented antibody and immediate PEGylation after antibody immobilization contributed to the formation of a high-performance SAP immunolatex.

摘要

兔抗人铁蛋白(anti-hFT)多克隆免疫球蛋白 G(IgG)和聚乙二醇(PEG)被顺序共固定在聚苯乙烯亚微米颗粒(sMPs)上,以构建 sMP/anti-hFT/PEG(SAP)免疫乳胶。在不同的 pH 值下进行抗 hFT 的化学固定,以评估抗原识别的变化。碱性 pH 不利于抗 hFT 与 sMPs 的结合,但与中性 pH 相比,显著增加了其抗原识别能力。我们通过评估抗体结合的动力学,包括固定、抗原识别和结合的抗 hFT 的取向的时间依赖性,进一步研究了这一有趣的现象。因此,我们将高抗原识别归因于碱性 pH 下 sMPs 和抗 hFT 之间的显著静电排斥,这主要阻止了抗 hFT 接近 sMPs,同时促进了适合抗原识别的抗 hFT 取向。随后的 PEG 修饰保持了这种抗 hFT 取向,如果没有这种取向,抗原可及的取向会随时间减少。因此,适当取向的抗体和抗体固定后的即时 PEG 化有助于形成高性能 SAP 免疫乳胶。

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