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古菌 Sac7d 支架蛋白对替代文库设计的耐受性:抗免疫球蛋白 G Affitins 的特性。

Tolerance of the archaeal Sac7d scaffold protein to alternative library designs: characterization of anti-immunoglobulin G Affitins.

机构信息

Université de Nantes, UMR CNRS 6204, Ingénierie de la reconnaissance, F-44322 Nantes, France.

出版信息

Protein Eng Des Sel. 2013 Apr;26(4):267-75. doi: 10.1093/protein/gzs106. Epub 2013 Jan 11.

DOI:10.1093/protein/gzs106
PMID:23315487
Abstract

Engineered protein scaffolds have received considerable attention as alternatives to antibodies in both basic and applied research, as they can offer superior biophysical properties often associated with a simpler molecular organization. Sac7d has been demonstrated as an effective scaffold for molecular recognition. Here, we used the initial L1 'flat surface' library constructed by randomization of 14 residues, to identify ligands specific for human immunoglobulin G. To challenge the plasticity of the Sac7d protein scaffold, we designed the alternative L2 'flat surface & loops' library whereof only 10 residues are randomized. Representative binders (Affitins) of the two libraries exhibited affinities in the low nanomolar range and were able to recognize different epitopes within human immunoglobulin G. These Affitins were stable up to pH 12 while largely conserving other favorable properties of Sac7d protein, such as high expression yields in Escherichia coli, solubility, thermal stability up to 80.7°C, and acidic stability (pH 0). In agreement with our library designs, mutagenesis study revealed two distinct binding areas, one including loops. Together, our results indicate that the Sac7d scaffold tolerates alternative library designs, which further expands the diversity of Affitins and may provide a general way to create tailored affinity tools for demanding applications.

摘要

工程化蛋白质支架作为抗体的替代品,在基础研究和应用研究中都受到了广泛关注,因为它们可以提供更优越的物理性质,通常与更简单的分子结构相关联。Sac7d 已被证明是一种有效的分子识别支架。在这里,我们使用最初通过随机化 14 个残基构建的 L1“平坦表面”文库,来鉴定与人免疫球蛋白 G 特异性结合的配体。为了挑战 Sac7d 蛋白质支架的可塑性,我们设计了替代的 L2“平坦表面和环”文库,其中只有 10 个残基被随机化。这两个文库的代表性结合物(Affitins)的亲和力均在纳摩尔范围内,并能够识别人免疫球蛋白 G 内的不同表位。这些 Affitins 在 pH 值为 12 时仍然稳定,同时在很大程度上保留了 Sac7d 蛋白质的其他有利特性,如在大肠杆菌中的高表达产量、可溶性、高达 80.7°C 的热稳定性和酸性稳定性(pH 值为 0)。与我们的文库设计一致,突变研究揭示了两个不同的结合区域,其中一个包括环。总之,我们的结果表明,Sac7d 支架可以耐受替代文库设计,这进一步扩展了 Affitins 的多样性,并可能为满足苛刻应用需求的定制亲和工具提供一种通用方法。

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