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Evaluation of Production Parameters with the Vaccinia Virus Expression System Using Microcarrier Attached HeLa Cells

机译:使用微载体附着的HeLa细胞通过牛痘病毒表达系统评估生产参数

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Parameters that affect production of the recombinant reporter protein,EGFP,in the T7 promoter based VOTE vaccinia virus-HeLa cell expression system were examined.Length of infection phase,inducer concentration,and timing of its addition relative to infection were evaluated in 6-well plate monolayer cultures.One hour infection with 1.0 mM IPTG added at the time of infection provided a robust process.For larger scale experiments,anchorage-dependent HeLa cells were grown on 5 g/L Cytodex 3 microcarriers.The change to this dynamic culture environment,with cell-covered microcarriers suspended in culture medium in spinner flasks,suggested a re-examination of the multiplicity of infection (MOI) for this culture type that indicated a need for an increase in the number of virus particles per cell to 5.0,higher than that needed for complete infection in monolayer tissue flask culture.Additionally,dissolved oxygen level and temperature during the protein production phase were evaluated for their effect on EGFP expression in microcarrier spinner flask culture.Both increased dissolved oxygen,based on surface area to volume (SA/V) adjustments,and decreased temperature from 37 to 31 deg C showed increases in EGFP production over the course of the production phase.The level of production achieved with this system reached approximately 17 mug EGFP/10~6 infected cells.
机译:在基于T7启动子的VOTE牛痘病毒-HeLa细胞表达系统中,研究了影响重组报告蛋白EGFP产生的参数。在6孔中评估了感染阶段的长度,诱导剂浓度以及添加时间相对于感染的时间。感染时添加1.0 mM IPTG一小时感染提供了一个强大的过程。对于大规模实验,锚固依赖性HeLa细胞在5 g / L Cytodex 3微载体上生长。 ,将带有细胞覆盖的微载体悬浮在旋转瓶中的培养基中,建议针对这种培养类型重新检查感染复数(MOI),这表明需要将每个细胞的病毒颗粒数量增加到5.0以上而不是单层组织培养瓶中完全感染所需要的。另外,还对蛋白质生产阶段的溶解氧水平和温度进行了评估。在微载体旋转培养瓶培养物中,EGFP的表达受到影响。基于表面积/体积(SA / V)的调整,溶解氧均增加,温度从37℃降低至31℃,这表明在生产阶段过程中EGFP的产量增加。用该系统达到的生产水平达到了约17个马克杯EGFP / 10〜6感染细胞。

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