Parsons Thomas B, Struwe Weston B, Gault Joseph, Yamamoto Keisuke, Taylor Thomas A, Raj Ritu, Wals Kim, Mohammed Shabaz, Robinson Carol V, Benesch Justin L P, Davis Benjamin G
Department of Chemistry, University of Oxford, Chemistry Research Laboratory, Mansfield Road, Oxford, OX1 3TA, UK.
Department of Pharmacology, University of Oxford, Oxford, OX1 3QT, UK.
Angew Chem Int Ed Engl. 2016 Feb 12;55(7):2361-7. doi: 10.1002/anie.201508723. Epub 2016 Jan 12.
Glycosylation patterns in antibodies critically determine biological and physical properties but their precise control is a significant challenge in biology and biotechnology. We describe herein the optimization of an endoglycosidase-catalyzed glycosylation of the best-selling biotherapeutic Herceptin, an anti-HER2 antibody. Precise MS analysis of the intact four-chain Ab heteromultimer reveals nonspecific, non-enzymatic reactions (glycation), which are not detected under standard denaturing conditions. This competing reaction, which has hitherto been underestimated as a source of side products, can now be minimized. Optimization allowed access to the purest natural form of Herceptin to date (≥90 %). Moreover, through the use of a small library of sugars containing non-natural functional groups, Ab variants containing defined numbers of selectively addressable chemical tags (reaction handles at Sia C1) in specific positions (for attachment of cargo molecules or "glycorandomization") were readily generated.
抗体中的糖基化模式关键地决定了生物学和物理性质,但其精确控制在生物学和生物技术领域是一项重大挑战。我们在此描述了一种内切糖苷酶催化畅销生物治疗药物赫赛汀(一种抗HER2抗体)糖基化的优化方法。对完整的四链抗体异源多聚体进行精确的质谱分析揭示了非特异性、非酶促反应(糖基化),这些反应在标准变性条件下无法检测到。这种迄今被低估为副产物来源的竞争反应现在可以被最小化。优化使得能够获得迄今为止最纯的天然形式的赫赛汀(≥90%)。此外,通过使用一个包含非天然官能团的小糖库,在特定位置(用于连接货物分子或“糖基随机化”)含有确定数量的可选择性寻址化学标签(唾液酸C1处的反应手柄)的抗体变体很容易产生。
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