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在组合蛋白质工程应用中,评估葡萄球菌细胞表面展示和流式细胞术用于亲和蛋白的筛选后表征。

Evaluation of staphylococcal cell surface display and flow cytometry for postselectional characterization of affinity proteins in combinatorial protein engineering applications.

作者信息

Löfblom John, Sandberg Julia, Wernérus Henrik, Ståhl Stefan

机构信息

School of Biotechnology, Royal Institute of Technology, AlbaNova University Center, SE-106 91 Stockholm, Sweden.

出版信息

Appl Environ Microbiol. 2007 Nov;73(21):6714-21. doi: 10.1128/AEM.01432-07. Epub 2007 Sep 14.

Abstract

For efficient generation of high-affinity protein-based binding molecules, fast and reliable downstream characterization platforms are needed. In this work, we have explored the use of staphylococcal cell surface display together with flow cytometry for affinity characterization of candidate affibody molecules directly on the cell surface. A model system comprising three closely related affibody molecules with different affinities for immunoglobulin G and an albumin binding domain with affinity for human serum albumin was used to investigate advantages and differences compared to biosensor technology in a side-by-side manner. Equilibrium dissociation constant (K(D)) determinations as well as dissociation rate analysis were performed using both methods, and the results show that the on-cell determinations give both K(D) and dissociation rate values in a very fast and reproducible manner and that the relative affinities are very similar to the biosensor results. Interestingly, the results also show that there are differences between the absolute affinities determined with the two different technologies, and possible explanations for this are discussed. This work demonstrates the advantages of cell surface display for directed evolution of affinity proteins in terms of fast postselectional, on-cell characterization of candidate clones without the need for subcloning and subsequent protein expression and purification but also demonstrates that it is important to be aware that absolute affinities determined using different methods often vary substantially and that such comparisons therefore could be difficult.

摘要

为了高效生成基于蛋白质的高亲和力结合分子,需要快速且可靠的下游表征平台。在这项工作中,我们探索了将葡萄球菌细胞表面展示与流式细胞术结合使用,以直接在细胞表面对候选亲和体分子进行亲和力表征。使用一个模型系统,该系统包含对免疫球蛋白G具有不同亲和力的三个密切相关的亲和体分子以及对人血清白蛋白具有亲和力的白蛋白结合域,以并排方式研究与生物传感器技术相比的优势和差异。使用这两种方法进行了平衡解离常数(K(D))测定以及解离速率分析,结果表明细胞表面测定能够以非常快速且可重复的方式给出K(D)和解离速率值,并且相对亲和力与生物传感器结果非常相似。有趣的是,结果还表明用两种不同技术测定的绝对亲和力之间存在差异,并对此进行了可能的解释。这项工作证明了细胞表面展示在亲和力蛋白质定向进化方面的优势,即能够在无需亚克隆以及后续蛋白质表达和纯化的情况下,对候选克隆进行快速的筛选后、细胞表面表征,但同时也表明必须意识到使用不同方法测定的绝对亲和力通常会有很大差异,因此这种比较可能会很困难。

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