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Metabolic control analysis of monoclonal antibody synthesis

机译:单克隆抗体合成的代谢控制分析

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A general route for protein synthesis in eukaryotic cells has been proposed and applied to monoclonal antibody (MAb) synthesis. It takes into account transcription of the gene, binding of ribosomes to mRNA, and polypeptide elongation including binding to SRP (signal recognition particles) and SRP-receptor, competing translocation, folding and glycosylation, assembly of the heavy and light chains in a tetrameric protein and Golgi processing and secretion. A comprehensive mode], was built on the basis of the proposed pathway. The model takes into account the mechanism of each step. Metabolic control analysis (MCA) principles were applied to the general pathway using the proposed model, and control coefficients were calculated. The results show a shared flux control (of both pathway flux and flux ratio at the branch) among different steps, i.e., transcription, folding, glycosylation, translocation and building blocks synthesis. The steps sharing the control depend on the concentration of building blocks, pathway flux and levels of OST (oligosacharyl transferase), BiP (heavy chain binding protein) and PDI (protein disulfide isomerase). Model predictions compare well with experimental data for MAb synthesis, explaining the control structure of the route and the heterogeneity of the product and also addressing future targets for improvement of the production rate of MAbs.
机译:已经提出了在真核细胞中蛋白质合成的一般途径,并将其应用于单克隆抗体(MAb)的合成。它考虑了基因的转录,核糖体与mRNA的结合以及包括与SRP(信号识别颗粒)和SRP受体结合,竞争性易位,折叠和糖基化,四聚体蛋白中重链和轻链组装在内的多肽延伸和高尔基体的加工和分泌。 [综合模式],是在提出的途径的基础上建立的。该模型考虑了每个步骤的机制。使用所提出的模型将代谢控制分析(MCA)原理应用于一般路径,并计算控制系数。结果显示了在不同步骤(即转录,折叠,糖基化,易位和构件合成)之间共享的通量控制(分支的通量和通量比)。共享控制的步骤取决于构件的浓度,途径通量和OST(寡糖基芳基转移酶),BiP(重链结合蛋白)和PDI(蛋白二硫键异构酶)的水平。模型预测与MAb合成的实验数据进行了很好的比较,解释了路线的控制结构和产品的异质性,还提出了提高MAb生产率的未来目标。

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