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首页> 外文期刊>Glycobiology. >Enhancing therapeutic glycoprotein production in Chinese hamster ovary cells by metabolic engineering endogenous gene control with antisense DNA and gene targeting.
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Enhancing therapeutic glycoprotein production in Chinese hamster ovary cells by metabolic engineering endogenous gene control with antisense DNA and gene targeting.

机译:通过反义DNA和基因靶向的代谢工程内源基因控制,增强中国仓鼠卵巢细胞的治疗性糖蛋白生产。

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摘要

Recombinant glycoprotein therapeutics have proven to be invaluable pharmaceuticals for the treatment of chronic and life-threatening diseases. Although these molecules are extraordinarily efficacious, many diseases have high dosage requirements of several hundred milligrams of protein for each administration. Multiple doses at this level are often required for treatment. One of the major challenges currently facing the biotechnology industry is the development of large-scale, cost-effective production and manufacturing processes of these biologically synthesized molecules. Metabolic engineering of animal cell expression hosts promises to address this challenge by substantially enhancing recombinant protein quality, productivity, and biological activity. In this report, we describe a novel approach to metabolic engineering in Chinese hamster ovary cells by control of endogenous gene expression. Analysis of the advantages and limitations of using antisense DNA and gene targeting as a means of control are discussed and several gene candidates for regulation with these techniques are identified. Practical considerations for using these technologies to reduce the levels of the CHO cell sialidase (Warner et al., Glycobiology, 3, 455-463, 1993) as a model gene system for regulation are also presented.
机译:重组糖蛋白疗法已被证明是治疗慢性和危及生命的疾病的宝贵药物。尽管这些分子非常有效,但许多疾病每次给药都需要数百毫克蛋白质的高剂量要求。通常需要在该水平上多次给药。生物技术行业当前面临的主要挑战之一是开发这些生物合成分子的大规模,经济高效的生产和制造工艺。动物细胞表达宿主的代谢工程有望通过大大提高重组蛋白的质量,生产率和生物活性来解决这一挑战。在这份报告中,我们描述了一种通过控制内源基因表达在中国仓鼠卵巢细胞中进行代谢工程的新方法。讨论了使用反义DNA和基因靶向作为控制手段的优缺点的分析,并确定了使用这些技术进行调控的几种候选基因。还提出了使用这些技术降低CHO细胞唾液酸酶水平的实际考虑(Warner等人,Glycobiology,3,455-463,1993),作为调节的模型基因系统。

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