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利用四嗪-苯乙烯环加成反应进行位点特异性抗体功能化。

Site-Specific Antibody Functionalization Using Tetrazine-Styrene Cycloaddition.

出版信息

Bioconjug Chem. 2018 May 16;29(5):1605-1613. doi: 10.1021/acs.bioconjchem.8b00114. Epub 2018 May 3.

Abstract

Biologics, such as antibody-drug conjugates, are becoming mainstream therapeutics. Consequently, methods to functionalize biologics without disrupting their native properties are essential for identifying, characterizing, and translating candidate biologics from the bench to clinical practice. Here, we present a method for site-specific, carboxy-terminal modification of single-chain antibody fragments (scFvs). ScFvs displayed on the surface of yeast were isolated and functionalized by combining intein-mediated expressed protein ligation (EPL) with inverse electron-demand Diels-Alder (IEDDA) cycloaddition using a styrene-tetrazine pair. The high thiol concentration required to trigger EPL can hinder the subsequent chemoselective ligation reactions; therefore, the EPL reaction was used to append styrene to the scFv, limiting tetrazine exposure to damaging thiols. Subsequently, the styrene-functionalized scFv was reacted with tetrazine-conjugated compounds in an IEDDA cycloaddition to generate functionalized scFvs that retain their native binding activity. Rapid functionalization of yeast surface-derived scFv in a site-directed manner could find utility in many downstream laboratory and preclinical applications.

摘要

生物制剂,如抗体药物偶联物,正在成为主流治疗方法。因此,在不破坏其天然特性的情况下对生物制剂进行功能化的方法对于从实验室到临床实践的候选生物制剂的鉴定、表征和转化至关重要。在这里,我们提出了一种用于单链抗体片段(scFv)的定点、羧基末端修饰的方法。通过将带有内含肽的表达蛋白连接(EPL)与使用苯乙烯-四嗪对的逆电子需求 Diels-Alder(IEDDA)环加成相结合,从酵母表面分离和功能化 scFv。触发 EPL 所需的高巯基浓度会阻碍随后的化学选择性连接反应;因此,EPL 反应被用来将苯乙烯附加到 scFv 上,限制四嗪暴露于破坏性巯基。随后,将苯乙烯功能化的 scFv 与四嗪缀合化合物在 IEDDA 环加成中反应,生成保留其天然结合活性的功能化 scFv。酵母表面衍生的 scFv 的快速定点功能化可能在许多下游实验室和临床前应用中具有实用价值。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f851/5963889/bcabe6ae5798/nihms966512f1.jpg

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