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Increased MSX level improves biological productivity and production stability in multiple recombinant GS CHO cell lines

机译:增加的MSX水平提高了多种重组GS Cho细胞系中的生物生产力和生产稳定性

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Increasing cell culture productivity of recombinant proteins via process improvements is the primary focus for research groups within biologics manufacturing. Any recommendations to improve a manufacturing process obviously must be effective, but also be robust, scalable, and with product quality comparable to the original process. In this study, we report that three different GS(-/-) CHO cell lines developed in media containing a standard concentration of the selection agent methionine sulfoximine (MSX), but then exposed to increased MSX concentrations during seed train expansion, achieved titer increases of 10-19%. This result was observed in processes already considerably optimized. Expanding the cells with a higher MSX concentration improved cell line production stability with increased culture age. Production cultures in 500-L and 1000-L bioreactors replicated laboratory results using 5-L bioreactors, demonstrating process robustness and scalability. Furthermore, product quality attributes of the final drug substance using the higher MSX process were comparable with those from cells expanded in media with the standard selection MSX concentration. Subsequent mechanistic investigations confirmed that the cells were not altered at the genetic level in terms of integration profiles or gene copy number, nor transcriptional levels of glutamine synthetase, heavy chain, or light chain genes. This study provides an effective and applicable strategy to improve the productivity of therapeutic proteins for biologics manufacturing.
机译:通过工艺改进的重组蛋白的细胞培养生产率增加是生物制造中的研究组的主要重点。任何提高制造过程的建议都明显必须有效,但也具有强大,可扩展,以及与原始过程相当的产品质量。在这项研究中,我们报告说,在含有标准浓度的选择剂甲硫氨嘧啶(MSX)的培养基中开发的三种不同的GS( - / - )CHO细胞系,但随后暴露于种子火车膨胀期间的MSX浓度增加,实现滴度增加10-19%。在已经大大优化的过程中观察到该结果。通过较高的MSX浓度扩展细胞改善了细胞系的产生稳定性随着培养年龄而增加。 500-L和1000-L生物反应器的生产培养物通过5-L生物反应器复制实验室结果,展示了过程鲁棒性和可扩展性。此外,使用较高的MSX工艺的最终药物物质的产品质量属性与来自培养基中膨胀的细胞的产品质量属性与标准选择MSX浓度相媲美。随后的机械研究证实,在整合谱或基因拷贝数,或谷氨酰胺合成酶,重链或轻链基因的转录水平,细胞没有在遗传水平上改变。本研究提供了一种有效且适用的策略,提高生物制造制造的治疗蛋白的生产率。

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