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Maximizing antibody production in a targeted integration host by optimization of subunit gene dosage and position

机译:通过优化亚基基因剂量和位置,最大化靶向整合宿主中的抗体产生

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Historically, therapeutic protein production in Chinese hamster ovary (CHO) cells has been accomplished by random integration (RI) of expression plasmids into the host cell genome. More recently, the development of targeted integration (TI) host cells has allowed for recombination of plasmid DNA into a predetermined genomic locus, eliminating one contributor to clone-to-clone variability. In this study, a TI host capable of simultaneously integrating two plasmids at the same genomic site was used to assess the effect of antibody heavy chain and light chain gene dosage on antibody productivity. Our results showed that increasing antibody gene copy number can increase specific productivity, but with diminishing returns as more antibody genes are added to the same TI locus. Random integration of additional antibody DNA copies in to a targeted integration cell line showed a further increase in specific productivity, suggesting that targeting additional genomic sites for gene integration may be beneficial. Additionally, the position of antibody genes in the two plasmids was observed to have a strong effect on antibody expression level. These findings shed light on vector design to maximize production of conventional antibodies or tune expression for proper assembly of complex or bispecific antibodies in a TI system.
机译:从历史上看,中国仓鼠卵巢(CHO)细胞中的治疗蛋白质产生已经通过将表达质粒的随机整合(RI)进入宿主细胞基因组来实现。最近,靶向整合(Ti)宿主细胞的发展已经允许将质粒DNA重组成预定的基因组轨迹,从而消除了一种克隆对克隆变异性的一个贡献者。在该研究中,使用能够在同一基因组位点同时整合两种质粒的Ti宿主来评估抗体重链和轻链基因剂量对抗体生产率的影响。我们的结果表明,增加抗体基因拷贝数可以提高比生产率增加,但随着更多抗体基因加入到相同的Ti基因座中,返回递减。附加抗体DNA的随机整合在靶向整合细胞系中拷贝显示出特异性生产率的进一步增加,表明靶向基因集成的额外基因组位点可能是有益的。另外,观察到两种质粒中的抗体基因的位置对抗体表达水平具有很强的影响。这些调查结果揭示了向量设计,以最大化常规抗体或调谐表达的产生,以便在TI系统中适当地组装复合物或双特异性抗体。

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