表面等离子共振
催交
背景(考古学)
抗体
化学
动力学
受体-配体动力学
离解常数
生物系统
纳米技术
材料科学
生物
免疫学
生物化学
物理
工程类
纳米颗粒
古生物学
受体
系统工程
量子力学
作者
Stephen Hearty,Paul Leonard,Hui Ma,Richard O’Kennedy
标识
DOI:10.1007/978-1-4939-8648-4_22
摘要
Surface plasmon resonance (SPR) is now widely embraced as a technology for monitoring a diverse range of protein-protein interactions and is considered almost de rigueur for characterizing antibody-antigen interactions. The technique obviates the need to label either of the interacting species, and the binding event is visualized in real time. Thus, it is ideally suited for screening crude, unpurified antibody samples that dominate early candidate panels following antibody selection campaigns. SPR returns not only concentration and affinity data but when used correctly can resolve the discrete component kinetic parameters (association and dissociation rate constants) of the affinity interaction. Herein, we outline some SPR-based generic antibody screening configurations and methodologies in the context of expediting data-rich ranking of candidate antibody panels and ensuring that antibodies with the optimal kinetic binding characteristics are reliably identified.
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