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体外使用未缀合的肽抗原进行抗体亲和力成熟。

Antibody affinity maturation in vitro using unconjugated peptide antigen.

机构信息

Department of Chemistry and Biotechnology, School of Engineering, The University of Tokyo, Tokyo, Japan.

出版信息

Protein Eng Des Sel. 2010 Apr;23(4):185-93. doi: 10.1093/protein/gzp093. Epub 2010 Feb 1.

Abstract

Selection of antibody library in vitro is almost always performed on a certain solid-phase with immobilized antigen. However, for the selection of small molecule binders, conjugation of the antigen to a carrier molecule is indispensable, which often leads to the selection of unwanted binders such as conjugate-binders or those with insufficient specificity. Here we describe a rapid and efficient way to improve the affinity of an anti-small molecule antibody without antigen derivatization. The method is based on the open-sandwich (OS) principle, which utilizes the antigen-dependent stabilization of antibody variable domain Fv. We used an anti-osteocalcin C-terminal peptide Fv that showed a good response but with moderate sensitivity in OS ELISA as a model. By selecting PCR-randomized V(H)-displaying phages for superior binders to the immobilized V(L) fragment in the presence of limited amount of antigen peptide, V(H) mutants that show superior detection sensitivity in OS ELISA were obtained, and were characterized to retain improved antigen-binding affinity. Furthermore, saturation mutagenesis of a mutant resulted in further improvement in sensitivity. This 'OS-selection' will be the first to select anti-small molecule antibodies without using conjugated antigens, and especially useful in the affinity maturation of antibodies whose Fv has limited stability in the absence of antigen.

摘要

体外抗体文库的选择几乎总是在固定有抗原的某种固相上进行。然而,对于小分子结合物的选择,抗原与载体分子的缀合是必不可少的,这往往导致选择不想要的结合物,如缀合结合物或特异性不足的结合物。在这里,我们描述了一种无需抗原衍生化即可提高抗小分子抗体亲和力的快速有效的方法。该方法基于开放式三明治(OS)原理,该原理利用了抗体可变区 Fv 对抗原依赖性的稳定化。我们使用了一种抗骨钙素 C 末端肽 Fv 作为模型,该 Fv 在 OS ELISA 中具有良好的反应性,但灵敏度中等。通过选择在有限量的抗原肽存在下对固定化 V(L)片段具有优异结合能力的 PCR 随机化 V(H)-展示噬菌体,获得了在 OS ELISA 中显示出优异检测灵敏度的 V(H)突变体,并对其进行了表征以保留改善的抗原结合亲和力。此外,对突变体进行饱和诱变可进一步提高灵敏度。这种“OS 选择”将首次用于选择不使用缀合抗原的抗小分子抗体,尤其适用于那些在没有抗原的情况下 Fv 稳定性有限的抗体的亲和力成熟。

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