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控制稳定转染 CHO 细胞中的 IgG LC:HC 比值及研究其对表达、聚集、糖基化和构象稳定性的影响。

Control of IgG LC:HC ratio in stably transfected CHO cells and study of the impact on expression, aggregation, glycosylation and conformational stability.

机构信息

Bioprocessing Technology Institute, Agency for Science, Technology and Research (A*STAR), 20 Biopolis Way, #06-01 Centros, Singapore 138668, Singapore.

出版信息

J Biotechnol. 2013 Jun 10;165(3-4):157-66. doi: 10.1016/j.jbiotec.2013.03.019. Epub 2013 Apr 10.

DOI:10.1016/j.jbiotec.2013.03.019
PMID:23583871
Abstract

Immunoglobulin G (IgG), the most common class of commercial monoclonal antibodies (mAbs), exists as multimers of two identical light chains (LC) and two identical heavy chains (HC) assembled together by disulfide bridges. Due to the kinetics of mAb assembly, it is suggested that expression of LC and HC in equal amounts is not optimal for IgG production. We designed a set of vectors using internal ribosome entry site (IRES) elements to control LC and HC expression. The intracellular LC:HC ratio of stable IgG expressing Chinese hamster ovary (CHO) cell pools can be controlled effectively at four different ratios of 3.43, 1.24, 1.12, and 0.32. The stable pools were used to study the impact of LC:HC ratio on mAb expression and quality. Gene amplification was most effective for pools with excess LC and generated the highest mAb titers among the transfected pools. When LC:HC ratio was greater than one, more than 97% of the secreted products were IgG monomers. The products also have similar N-glycosylation profiles and conformational stabilities at those ratios. For pools presented a lower LC:HC ratio of 0.32, monomers only constituted half of the product with the other half being aggregates and mAb fragments. High mannose-type N-glycans increased while fucosylated and galactosylated glycans decreased significantly at the lowest LC:HC ratio. Product stability was also adversely affected. The results obtained provide insights to the impact of different LC:HC ratios on stable mAb production and useful information for vector design during generation of mAb producing cell lines.

摘要

免疫球蛋白 G(IgG)是最常见的商业单克隆抗体(mAb)类别,由两条相同的轻链(LC)和两条相同的重链(HC)通过二硫键组装而成的多聚体。由于 mAb 组装的动力学特性,建议等量表达 LC 和 HC 对于 IgG 生产并不是最佳的。我们设计了一组使用内部核糖体进入位点(IRES)元件来控制 LC 和 HC 表达的载体。稳定表达 IgG 的中国仓鼠卵巢(CHO)细胞池的细胞内 LC:HC 比值可以有效地控制在 3.43、1.24、1.12 和 0.32 四个不同的比值。稳定池被用于研究 LC:HC 比值对 mAb 表达和质量的影响。基因扩增对于 LC 过量的池最有效,并在转染池中产生最高的 mAb 滴度。当 LC:HC 比值大于 1 时,超过 97%的分泌产物是 IgG 单体。在这些比值下,产物还具有相似的 N-糖基化谱和构象稳定性。对于 LC:HC 比值较低的 0.32 的池,单体仅构成产物的一半,另一半是聚集体和 mAb 片段。在最低的 LC:HC 比值下,高甘露糖型 N-聚糖增加,而岩藻糖基化和半乳糖基化聚糖显著减少。产物稳定性也受到不利影响。所得结果提供了不同 LC:HC 比值对稳定 mAb 生产的影响的深入了解,并为产生 mAb 产生细胞系的载体设计提供了有用的信息。

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