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微型抗体:利用两亲性螺旋在大肠杆菌中产生具有高亲和力的功能性、柔性连接的二聚体FV片段。

Miniantibodies: use of amphipathic helices to produce functional, flexibly linked dimeric FV fragments with high avidity in Escherichia coli.

作者信息

Pack P, Plückthun A

机构信息

Genzentrum Universität München, Max-Planck-Institut für Biochemie, Martinsried, FRG.

出版信息

Biochemistry. 1992 Feb 18;31(6):1579-84. doi: 10.1021/bi00121a001.

Abstract

We have designed dimeric antibody fragments that assemble in Escherichia coli. They are based on single-chain FV fragments, with a flexible hinge region from mouse IgG3 and an amphiphilic helix fused to the C-terminus of the antibody fragment. The sequence of the helix was taken either from that of a previously reported four-helix bundle design or from a leucine zipper, optionally extended with a short cysteine-containing peptide. The bivalent fragments associate in vivo, either with covalent linkage or with a monomer-dimer equilibrium, and results from ultracentrifugation sedimentation studies and SDS-PAGE are consistent with dimers. All constructs are able to bind to surface-bound antigen under conditions in which only bivalent but not monovalent antibody fragments bind. The covalent bundle helix construct shows binding characteristics nearly identical to those of the much larger whole mouse antibody, resulting in substantially more stable immunoglobulin-antigen complexes than in the case of monovalent fragments. This modular design of natural and engineered protein domains directly leads to a boost of avidity, and it allows the construction of bispecific antibody fragments in functional form in E. coli.

摘要

我们设计了可在大肠杆菌中组装的二聚体抗体片段。它们基于单链FV片段,带有来自小鼠IgG3的柔性铰链区以及融合到抗体片段C末端的两亲性螺旋。螺旋序列要么取自先前报道的四螺旋束设计,要么取自亮氨酸拉链,并可选择地用短的含半胱氨酸肽进行延伸。二价片段在体内以共价连接或单体-二聚体平衡的方式缔合,超速离心沉降研究和SDS-PAGE的结果与二聚体一致。所有构建体在仅二价而非单价抗体片段结合的条件下都能够结合表面结合的抗原。共价束螺旋构建体显示出与大得多的完整小鼠抗体几乎相同的结合特性,与单价片段相比,产生的免疫球蛋白-抗原复合物要稳定得多。天然和工程化蛋白质结构域的这种模块化设计直接导致亲和力的提高,并且允许在大肠杆菌中构建功能形式的双特异性抗体片段。

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