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首页> 外文期刊>Vaccine >Microcarrier-based MDCK cell culture system for the production of influenza H5N1 vaccines.
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Microcarrier-based MDCK cell culture system for the production of influenza H5N1 vaccines.

机译:基于微载体的MDCK细胞培养系统,用于生产H5N1流感疫苗。

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Current egg-based influenza vaccine production technology, which is labor intensive and slow, would not be able to meet demand during an influenza pandemic. Thus, interest in the emerging technology of using mammalian cells for vaccine production has been great. In this study, Madin-Darby canine kidney (MDCK) cells using microcarrier culture systems were established to produce inactivated whole-virus H5N1 vaccine. The current clade-1 influenza H5N1 vaccine virus (NIBRG-14) was provided by the UK National Institute for Biological Standards and Control. Various process parameters were first optimized in 100-mL scale spinner flasks then scaled up to a 1-L scale bioreactor system. In the 1-L scale bioreactor system, peak virus titer could reach 10(8-9)TCID(50)/mL using serum-containing medium. After purification and inactivation, hemagglutinin (HA) protein content reached 31.56-43.96mug/mL in two different runs. In mice immunogenicity studies, two doses of the purified vaccine antigen adjuvanted with aluminum phosphate induced good immune responses in 0.2 and 1.0mug HA dosages (geometric mean titers of hemagglutination-inhibition antibody: 113 and 242, respectively). This study demonstrates the feasibility of the development of MDCK cell-based inactivated influenza H5 vaccines in microcarrier culture systems and could be valuable to many countries that are planning to establish manufacturing capacity for influenza vaccines.
机译:当前的蛋基流感疫苗生产技术劳动强度大且速度慢,无法满足流感大流行期间的需求。因此,对于使用哺乳动物细胞生产疫苗的新兴技术的兴趣很大。在这项研究中,使用微载体培养系统建立了Madin-Darby犬肾(MDCK)细胞以生产灭活的全病毒H5N1疫苗。当前的进化枝1型流感H5N1疫苗病毒(NIBRG-14)由英国国家生物标准与控制研究所提供。首先在100 mL规模的旋转瓶中优化各种工艺参数,然后扩大至1 L规模的生物反应器系统。在1-L规模的生物反应器系统中,使用含血清的培养基,病毒滴度峰值可以达到10(8-9)TCID(50)/ mL。纯化和灭活后,血凝素(HA)蛋白质含量在两次不同的运行中均达到31.56-43.96mug / mL。在小鼠免疫原性研究中,佐以磷酸铝的两剂纯化疫苗抗原以0.2和1.0杯HA剂量诱导了良好的免疫反应(血凝抑制抗体的几何平均滴度分别为113和242)。这项研究证明了在微载体培养系统中开发基于MDCK细胞的灭活H5流感疫苗的可行性,这对于许多计划建立流感疫苗生产能力的国家可能是有价值的。

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