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Cell growth arrest by nucleotides, nucleosides and bases as a tool for improved production of recombinant proteins

机译:核苷酸,核苷和碱基阻止细胞生长,作为改善重组蛋白生产的工具

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Arresting cell growth and thus decreasing cell division potentially lessens the chance for genetic drift in the cell population; this would be of utmost importance for the consistent production of biopharmaceuticals during long periods. The drawback of the addition of well-known synchronizing agents, such as chemotherapeutics, is that they cause a disproportionate accumulation of cellular constituents, leading to cell death. The use of compounds that are naturally synthesized by the cell, as is the case of nucleotides, nucleosides, and bases (Nt/Ns/B), is shown in this work to be a promising tool. The addition of purines and pyrimidines was tested using a CHO cell line producing the secreted form of the human placental alkaline phosphatase enzyme (SEAP). From the chemical alternatives tested, AMP was the most promising compound for protein production improvement; it reduced cell growth and maintained the culture with high cell viability for long periods, while increasing SEAP specific productivity 3-fold. The use of CHO and BHK mammalian cells producing Factor VII and the use of a insect cell line (Sf9) showed that the effect of AMP addition seems to be independent of the r-protein and cell line. With the addition of AMP, accumulation of cells at the S phase was accompanied by an increase of the protein specific productivity. Addition of known synchronizing drugs (aphidicolin and doxorubicin) and application of environmental cell growth arrest strategies (depletion of nutrients and byproduct accumulation) showed also to effectively arrest CHO cell growth. A careful look onto cell cycle distribution in the different scenarios created, shows whether it is important to consider r-protein expression dependency upon cell cycle in process optimization and operation strategies.
机译:阻止细胞生长从而减少细胞分裂可能会减少细胞群体中遗传漂移的机会;这对于长期稳定生产生物药品至关重要。添加众所周知的同步剂(例如化学治疗剂)的缺点是它们会引起细胞成分不成比例的积累,从而导致细胞死亡。这项工作表明,使用细胞天然合成的化合物(如核苷酸,核苷和碱基(Nt / Ns / B))是一种很有前途的工具。使用产生人胎盘碱性磷酸酶(SEAP)分泌形式的CHO细胞系测试嘌呤和嘧啶的添加。从测试的化学替代品来看,AMP是改善蛋白质生产的最有前途的化合物。它减少了细胞的生长,并长期保持培养物具有高细胞活力,同时将SEAP的比生产率提高了3倍。使用产生因子VII的CHO和BHK哺乳动物细胞以及使用昆虫细胞系(Sf9)表明,添加AMP的作用似乎与r蛋白和细胞系无关。添加AMP后,S期细胞的积累伴随着蛋白质比生产率的提高。添加已知的同步药物(两性霉素和阿霉素)和应用环境细胞生长抑制策略(营养物质耗尽和副产物积累)也显示可以有效抑制CHO细胞生长。仔细观察在创建的不同场景中的细胞周期分布,可以看出在过程优化和操作策略中考虑r蛋白表达对细胞周期的依赖性是否重要。

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