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Custom made inclusion bodies: impact of classical process parameters and physiological parameters on inclusion body quality attributes

机译:定制包涵体:古典过程参数和生理参数对包涵体质量属性的影响

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Abstract Background The bacterium E. coli is a major host for recombinant protein production of non-glycosylated products. Depending on the expression strategy, the recombinant protein can be located intracellularly. In many cases the formation of inclusion bodies (IBs), protein aggregates inside of the cytoplasm of the cell, is favored in order to achieve high productivities and to cope with toxic products. However, subsequent downstream processing, including homogenization of the cells, centrifugation or solubilization of the IBs, is prone to variable process performance or can be characterized by low extraction yields as published elsewhere. It is hypothesized that variations in IB quality attributes (QA) are responsible for those effects and that such attributes can be controlled by upstream process conditions. This contribution is aimed at analyzing how standard process parameters, such as pH and temperature (T) as well as different controlled levels of physiological parameters, such as specific substrate uptake rates, can vary IB quality attributes. Results Classical process parameters like pH and T influence the expression of analyzed IB. The effect on the three QAs titer, size and purity could be successfully revealed. The developed data driven model showed that low temperatures and low pH are favorable for the expression of the two tested industrially relevant proteins. Based on this knowledge, physiological control using specific substrate feeding rate (of glucose) qs,Glu is altered and the impact is tested for one protein. Conclusions Time dependent monitoring of IB QA—titer, purity, IB bead size—showed a dependence on classical process parameters pH and temperature. These findings are confirmed using a second industrially relevant strain. Optimized process conditions for pH and temperature were used to determine dependence on the physiological parameters, the specific substrate uptake rate (qs,Glu). Higher qs,Glu were shown to have a strong influence on the analyzed IB QAs and drastically increase the titer and purity in early time stages. We therefore present a novel approach to modulate—time dependently—quality attributes in upstream processing to enable robust downstream processing.
机译:摘要背景细菌大肠杆菌是用于重组蛋白质生产的非糖基化产品的主要主机。根据不同的表达方式,重组蛋白可以位于细胞内。在许多情况下包涵体(IBS),所述细胞的细胞质中的蛋白质内聚集体的形成,是为了实现高的生产率和以应付有毒产品青睐。然而,随后的下游加工,包括IBS的细胞,离心分离或溶解的均质化,容易产生可变的工艺性能或可通过低提取率被表征为别处发表。据推测,在IB质量属性(QA)的变化是负责这些效果并且这些属性可以由上游工艺条件来控制。这种贡献的目的是分析标准工艺参数,例如pH值和温度(T),以及生理参数的不同控制水平,如吸收速率特异性底物如何,可以改变IB质量属性。如pH和T的结果古典工艺参数影响分析IB的表达。这三个质量检查的滴度,大小和纯度的影响可以成功地显露出来。驱动模型的开发的数据表明,低的温度和低pH值对于两个的测试工业相关的蛋白质的表达是有利的。基于这一认识,生理控制使用特定的底物进料速率适量(葡萄糖),谷氨酸被改变从而冲击被用于一种蛋白质进行测试。结论时间IB QA-滴度,纯度的相关监测,IB珠尺寸显示对经典的工艺参数的pH值和温度的依赖性。这些发现使用第二工业相关应变证实。对pH和温度的优化工艺条件被用来确定关于生理参数,特定底物吸收率(适量,谷氨酸)依赖性。更高的Q,谷氨酸显示出对分析IB质量检查的强大的影响力,并大幅增加在早期阶段的效价和纯度。因此,我们提出了一种新颖的方法来调制时间依赖性质量属性在上游处理等,可稳定下游处理。

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