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Analysis of intracellular IgG secretion in Chinese hamster ovary cells to improve IgG production

机译:中国仓鼠卵巢细胞细胞内IgG分泌分析改善IgG产量

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The production of biopharmaceutical immunoglobulin G (IgG) using cultured mammalian cells, especially Chinese hamster ovary (CHO) cells is well established and has been markedly improved through the modification of cells and cell culture engineering technologies. The establishment of high-production cell lines remains a challenge. The intracellular secretion of IgG has been investigated to identify and solve the rate-limiting steps in antibody production. However, strategies that regulate the expression of proteins that are related to antibody secretory pathway have not consistently improved their production. In this study, key features and limitations of the antibody secretion process in recombinant CHO cells were analyzed to develop more efficient approaches for establishing high-production cells. By chase assay with protein translation inhibitors, IgG secretion reached a plateau when at least 20% of IgG remained in the cells. The secretion kinetics and retention ratio of IgG varied between IgG subclasses (two types of IgG1 and an IgG3 subclass). Immunofluorescent microscopy and size exclusion chromatography showed that the remaining intracellular IgG localized mainly within the endoplasmic reticulum (ER) and less with the cis-Golgi network, despite the formation of fully assembled IgG. These results show that remaining intracellular IgG is a target for enhancing antibody secretion, even in high-production CHO cells.
机译:使用培养的哺乳动物细胞生产生物制药免疫球蛋白G(IgG),特别是中国仓鼠卵巢(CHO)细胞,通过细胞和细胞培养工程技术的改性明显改善。建立高产细胞系仍然是一个挑战。已经研究了IgG的细胞内分泌以识别和解决抗体产生的速率限制步骤。然而,调节与抗体分泌途径相关的蛋白质表达的策略并未始终改善其生产。在该研究中,分析了重组CHO细胞中抗体分泌过程的关键特征和局限性,以产生更有效的建立高产量细胞的方法。通过用蛋白质翻译抑制剂追踪测定,当在细胞中至少20%的IgG中,IgG分泌达到高原。 IgG的分泌动力学和保留比在IgG亚类(两种IgG1和IgG3亚类)之间变化。尽管形成完全组装的IgG,但免疫荧光显微镜和尺寸排阻色谱显示主要在内质网(ER)和较少的内质子网上局部局部局部地局部地局部地局部。这些结果表明,即使在高产量CHO细胞中,剩余的细胞内IgG也是增强抗体分泌的靶标。

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