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Improving the batch-to-batch reproducibility in microbial cultures during recombinant protein production by guiding the process along a predefined total biomass profile

机译:通过沿预定的总生物量图谱引导过程提高重组蛋白生产过程中微生物培养中批次间的可重复性

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摘要

In industry Escherichia coli is the preferred host system for the heterologous biosynthesis of therapeutic proteins that do not need posttranslational modifications. In this report, the development of a robust high-cell-density fed-batch procedure for the efficient production of a therapeutic hormone is described. The strategy is to guide the process along a predefined profile of the total biomass that was derived from a given specific growth rate profile. This profile might have been built upon experience or derived from numerical process optimization. A surprisingly simple adaptive procedure correcting for deviations from the desired path was developed. In this way the batch-to-batch reproducibility can be drastically improved as compared to the process control strategies typically applied in industry. This applies not only to the biomass but, as the results clearly show, to the product titer also.
机译:在工业中,大肠杆菌是不需要翻译后修饰的治疗性蛋白质异源生物合成的优选宿主系统。在该报告中,描述了用于有效生产治疗激素的强大的高细胞密度补料分批程序的开发。该策略是沿着从给定的特定生长速率分布图导出的总生物量的预定义分布图来指导该过程。此配置文件可能是基于经验建立的,或者是从数值过程优化中得出的。开发了一种出人意料的简单自适应程序,用于校正与所需路径的偏差。通过这种方式,与工业上通常使用的过程控制策略相比,批次间的可重复性可以大大提高。这不仅适用于生物质,而且如结果清楚地显示,还适用于产品滴定度。

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