首页> 外文期刊>The Analyst: The Analytical Journal of the Royal Society of Chemistry: A Monthly International Publication Dealing with All Branches of Analytical Chemistry >Rapid and improved characterization of therapeutic antibodies and antibody related products using IdeS digestion and subunit analysis
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Rapid and improved characterization of therapeutic antibodies and antibody related products using IdeS digestion and subunit analysis

机译:使用IdeS酶切和亚基分析快速,改进地表征治疗性抗体和抗体相关产品

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摘要

The immunoglobulin degrading enzyme from Streptococcus pyogenes, IdeS, was discovered as a mechanism by which pathogenic bacteria circumvent antibody mediated immune defense. IdeS was found to rapidly and specifically cleave IgG into F(ab')2 and Fc/2 fragments. The enzymatic specificity has led to a range of recent developments in the analytical strategies for characterization of monoclonal therapeutic antibodies and related products such as antibody-drug conjugates, bispecific antibodies, antibody mixtures and Fc-fusion proteins. In this review article we describe the discovery and properties of IdeS, discuss the current challenges in characterizing antibody therapeutics and review the methodologies using IdeS to improve the characterization of therapeutic antibodies. The review is focused on critical quality attributes of the final antibody product as studied by IdeS fragmentation such as Fab- and Fc-glycosylation, oxidation, glycation, C-terminal lysine and others. In summary, this review presents a wide range of IdeS-based applications for improved characterization of originator, biosimilar and next generation antibody-based therapeutics.
机译:发现化脓性链球菌的免疫球蛋白降解酶IdeS是病原菌规避抗体介导的免疫防御的机制。发现IdeS能快速,特异性地将IgG裂解为F(ab')2和Fc / 2片段。酶特异性已导致表征单克隆治疗性抗体和相关产品(例如抗体-药物偶联物,双特异性抗体,抗体混合物和Fc融合蛋白)的分析策略的一系列最新发展。在这篇综述文章中,我们描述了IdeS的发现和性质,讨论了表征抗体治疗剂的当前挑战,并回顾了使用IdeS改进治疗性抗体表征的方法。审查的重点是通过IdeS片段研究的最终抗体产品的关键质量属性,例如Fab和Fc糖基化,氧化,糖基化,C端赖氨酸等。总而言之,本综述介绍了多种基于IdeS的应用,以改善对始发者,生物仿制药和下一代基于抗体的治疗剂的表征。

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