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针对人源治疗性 Fc 支架的高度选择性 IgNAR 可变单结构域的分离及其作为定制化生物工艺试剂的应用。

Isolation of highly selective IgNAR variable single-domains against a human therapeutic Fc scaffold and their application as tailor-made bioprocessing reagents.

机构信息

Elasmogen Ltd, Liberty Building, Foresterhill Health Campus, Foresterhill Road, Aberdeen AB25 2ZP, UK.

Merck Biopharma KGaA, Protein Engineering & Antibody Technologies, Global Research and Development, Frankfurter Str. 250 Darmstadt 64293, Germany.

出版信息

Protein Eng Des Sel. 2019 Dec 31;32(9):385-399. doi: 10.1093/protein/gzaa002.

DOI:10.1093/protein/gzaa002
PMID:32119084
Abstract

The adaptive immune system of cartilaginous fish (Elasmobranchii), comprising of classical hetero-tetrameric antibodies, is enhanced through the presence of a naturally occurring homodimeric antibody-like immunoglobulin-the new antigen receptor (IgNAR). The binding site of the IgNAR variable single-domain (VNAR) offers advantages of reduced size (<1/10th of classical immunoglobulin) and extended binding topographies, making it an ideal candidate for accessing cryptic epitopes otherwise intractable to conventional antibodies. These attributes, coupled with high physicochemical stability and amenability to phage display, facilitate the selection of VNAR binders to challenging targets. Here, we explored the unique attributes of these single domains for potential application as bioprocessing reagents in the development of the SEED-Fc platform, designed to generate therapeutic bispecific antibodies. A panel of unique VNARs specific to the SEED homodimeric (monospecific) 'by-products' were isolated from a shark semi-synthetic VNAR library via phage display. The lead VNAR candidate exhibited low nanomolar affinity and superior selectivity to SEED homodimer, with functionality being retained upon exposure to extreme physicochemical conditions that mimic their applicability as purification agents. Ultimately, this work exemplifies the robustness of the semi-synthetic VNAR platform, the predisposition of the VNAR paratope to recognise novel epitopes and the potential for routine generation of tailor-made VNAR-based bioprocessing reagents.

摘要

软骨鱼(软骨鱼纲)的适应性免疫系统,由经典的异四聚体抗体组成,通过存在天然同源二聚体抗体样免疫球蛋白 - 新抗原受体(IgNAR)得到增强。IgNAR 的可变单结构域(VNAR)的结合位点具有体积小(<经典免疫球蛋白的 1/10)和扩展结合形貌的优势,使其成为访问隐藏表位的理想候选物,而这些表位对传统抗体来说是难以捉摸的。这些特性,加上高物理化学稳定性和对噬菌体展示的适应性,有利于选择 VNAR 结合物来应对具有挑战性的目标。在这里,我们探索了这些单结构域的独特属性,以作为 SEED-Fc 平台开发中的生物加工试剂的潜在应用,该平台旨在生成治疗性双特异性抗体。通过噬菌体展示,从鲨鱼半合成 VNAR 文库中分离出一组针对 SEED 同源二聚体(单特异性)“副产物”的独特 VNAR。领先的 VNAR 候选物表现出低纳摩尔亲和力和对 SEED 同源二聚体的优异选择性,并且在暴露于模拟其作为纯化剂适用性的极端物理化学条件下保留功能。最终,这项工作体现了半合成 VNAR 平台的稳健性、VNAR 变构位识别新表位的倾向以及常规生成定制化 VNAR 基生物加工试剂的潜力。

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Methods Mol Biol. 2022;2446:19-33. doi: 10.1007/978-1-0716-2075-5_2.