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多组学揭示半胱氨酸补料浓度及其导致的氧化还原失衡对 CHO 细胞生物工艺中细胞能量代谢和特定产物生成的影响。

Multi-Omics Reveals Impact of Cysteine Feed Concentration and Resulting Redox Imbalance on Cellular Energy Metabolism and Specific Productivity in CHO Cell Bioprocessing.

机构信息

Cell Culture Development, Biogen Inc., Cambridge, MA, 02142, USA.

Department of Chemistry and Chemical Biology, Barnett Institute of Chemical and Biological Analysis, Northeastern University, Boston, MA, 02115, USA.

出版信息

Biotechnol J. 2020 Aug;15(8):e1900565. doi: 10.1002/biot.201900565. Epub 2020 Apr 3.

Abstract

Chinese hamster ovary (CHO) cells are currently the primary host cell lines used in biotherapeutic manufacturing of monoclonal antibodies (mAbs) and other biopharmaceuticals. Cellular energy metabolism and endoplasmic reticulum (ER) stress are known to greatly impact cell growth, viability, and specific productivity of a biotherapeutic; but the molecular mechanisms are not fully understood. The authors previously employed multi-omics profiling to investigate the impact of a reduction in cysteine (Cys) feed concentration in a fed-batch process and found that disruption of the redox balance led to a substantial decline in cell viability and titer. Here, the multi-omics findings are expanded, and the impact redox imbalance has on ER stress, mitochondrial homeostasis, and lipid metabolism is explored. The reduced Cys feed activates the amino acid response (AAR), increases mitochondrial stress, and initiates gluconeogenesis. Multi-omics analysis reveals that together, ER stress and AAR signaling shift the cellular energy metabolism to rely primarily on anaplerotic reactions, consuming amino acids and producing lactate, to maintain energy generation. Furthermore, the pathways are demonstrated in which this shift in metabolism leads to a substantial decline in specific productivity and altered mAb glycosylation. Through this work, meaningful bioprocess markers and targets for genetic engineering are identified.

摘要

中国仓鼠卵巢(CHO)细胞是目前生物治疗单抗(mAb)和其他生物制药生产中主要使用的宿主细胞系。众所周知,细胞能量代谢和内质网(ER)应激会极大地影响生物治疗剂的细胞生长、活力和比生产率;但分子机制尚不完全清楚。作者先前采用多组学分析来研究补料分批过程中半胱氨酸(Cys)进料浓度降低对细胞生长、活力和比生产率的影响,发现氧化还原平衡的破坏导致细胞活力和滴度显著下降。在这里,扩展了多组学发现,并探讨了氧化还原失衡对 ER 应激、线粒体稳态和脂质代谢的影响。减少的 Cys 进料会激活氨基酸反应(AAR),增加线粒体应激,并启动糖异生。多组学分析表明,内质网应激和 AAR 信号共同将细胞能量代谢转变为主要依赖于氨酰基反应,消耗氨基酸并产生乳酸,以维持能量产生。此外,还证明了这种代谢转变如何导致比生产率大幅下降和 mAb 糖基化改变的途径。通过这项工作,确定了有意义的生物工艺标志物和遗传工程靶点。

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