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A Markov chain model for N-linked protein glycosylation - towards a low-parameter tool for model-driven glycoengineering

机译:用于N-连接蛋白糖基化的Markov链模型-面向模型驱动糖工程的低参数工具

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摘要

Glycosylation is a critical quality attribute of most recombinant biotherapeutics. Consequently, drug development requires careful control of glycoforms to meet bioactivity and biosafety requirements. However, glycoengineering can be extraordinarily difficult given the complex reaction networks underlying glycosylation and the vast number of different glycans that can be synthesized in a host cell. Computational modeling offers an intriguing option to rationally guide glycoengineering, but the high parametric demands of current modeling approaches pose challenges to their application. Here we present a novel low-parameter approach to describe glycosylation using flux-balance and Markov chain modeling. The model recapitulates the biological complexity of glycosylation, but does not require userprovided kinetic information. We use this method to predict and experimentally validate glycoprofiles on EPO, IgG as well as the endogenous secretome following glycosyltransferase knock-out in different Chinese hamster ovary (CHO) cell lines. Our approach offers a flexible and user-friendly platform that can serve as a basis for powerful computational engineering efforts in mammalian cell factories for biopharmaceutical production. (C) 2015 International Metabolic Engineering Society. Published by Elsevier Inc. All rights reserved.
机译:糖基化是大多数重组生物治疗药物的关键质量属性。因此,药物开发需要仔细控制糖型以满足生物活性和生物安全性要求。但是,鉴于糖基化背后的复杂反应网络以及宿主细胞中可以合成的大量不同聚糖,因此糖工程改造可能异常困难。计算建模为合理地指导糖工程提供了一个有趣的选择,但是当前建模方法的高参数要求对其应用提出了挑战。在这里,我们提出一种新颖的低参数方法来描述使用通量平衡和马尔可夫链建模的糖基化。该模型概括了糖基化的生物学复杂性,但不需要用户提供动力学信息。我们使用这种方法来预测和实验验证在不同的中国仓鼠卵巢(CHO)细胞系中糖基转移酶敲除后EPO,IgG和内源性分泌组的糖谱。我们的方法提供了一个灵活且用户友好的平台,可以作为哺乳动物细胞工厂中用于生物制药生产的强大计算工程工作的基础。 (C)2015年国际代谢工程学会。由Elsevier Inc.出版。保留所有权利。

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