通过加速共轭后水解优化用于天然抗体偶联的二溴马来酰亚胺（DBM）平台。

Optimisation of the dibromomaleimide (DBM) platform for native antibody conjugation by accelerated post-conjugation hydrolysis.

作者信息

Morais Maurício, Nunes João P M, Karu Kersti, Forte Nafsika, Benni Irene, Smith Mark E B, Caddick Stephen, Chudasama Vijay, Baker James R

机构信息

Department of Chemistry, UCL, 20 Gordon St, London, UK WC1H 0AJ.

出版信息

Org Biomol Chem. 2017 Apr 5;15(14):2947-2952. doi: 10.1039/c7ob00220c.

DOI:10.1039/c7ob00220c

PMID:28290574

Abstract

Disulfide bridging offers a convenient approach to generate site-selective antibody conjugates from native antibodies. To optimise the reagents available to achieve this strategy, we describe here the use of dibromomaleimides designed to undergo accelerated post-conjugation hydrolysis. Conjugation and hydrolysis, which serve to 'lock' the conjugates as robustly stable maleamic acids, is achieved in just over 1 h. This dramatic acceleration is also shown to infer significant improvements in homogeneity, as demonstrated by mass spectrometry analysis.

摘要

二硫键桥接提供了一种从天然抗体生成位点选择性抗体缀合物的便捷方法。为了优化用于实现该策略的试剂，我们在此描述了二溴马来酰亚胺的使用，其设计用于在缀合后加速水解。缀合和水解过程可在1小时多一点的时间内将缀合物“锁定”为非常稳定的马来酰胺酸，质谱分析表明，这种显著的加速还带来了均一性的显著提高。

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通过加速共轭后水解优化用于天然抗体偶联的二溴马来酰亚胺（DBM）平台。

Optimisation of the dibromomaleimide (DBM) platform for native antibody conjugation by accelerated post-conjugation hydrolysis.

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