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首页> 外文期刊>Virology >MICROEVOLUTION OF TYPE 3 SABIN STRAIN OF POLIOVIRUS IN CELL CULTURES AND ITS IMPLICATIONS FOR ORAL POLIOVIRUS VACCINE QUALITY CONTROL
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MICROEVOLUTION OF TYPE 3 SABIN STRAIN OF POLIOVIRUS IN CELL CULTURES AND ITS IMPLICATIONS FOR ORAL POLIOVIRUS VACCINE QUALITY CONTROL

机译:脊髓灰质炎3型沙宾菌在细胞培养中的微进化及其对口腔脊髓灰质炎疫苗质量控制的意义

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摘要

Screening for sequence heterogeneities in Sabin Type 3 strains of attenuated poliovirus demonstrated mutations that consistently accumulate to significant levels following 10 passages in cultures of primary African green monkey kidney (AGMK) cells or continuous cultures of Vero cells. Fourteen newly identified mutations were quantified by mutant analysis by PCR and restriction enzyme cleavage in passages and in batches of commercial vaccines made in AGMK and Vero cells from the Sabin original (SO) seed virus and from a seed virus rederived by RNA plaque purification (RSO or ''Pfizer'' seed). Nine of the 14 mutations were reproducibly observed in more than one series of passages. Although 5 other mutations were observed in only one set of passages each, their content gradually increased to a high percentage, suggesting that all the mutations that we found accumulated consistently. SO-derived samples accumulated more mutations than did RSO-derived ones, and the number of mutations and the rates of their accumulation were higher in Vero than in AGMK cells. While the rates of accumulation of most mutations were higher when passaging was performed at 37 degrees, a U --> C transition at nucleotide 5832 occurred faster at 34 degrees, the temperature used for vaccine production. Analysis of Type 3 oral poliovirus vaccine (OPV) monopools made by six manufacturers found only 5 of these newly identified mutations in Vaccine batches (nucleotides 3956, 4935, 5357, 5788, and 5832). Some of the mutations were found in trace amounts (less than 0.1%) while others were present at up to 1.8% levels, The pattern of these mutations was characteristic for the type of seed virus and the cell substrate but demonstrated no correlation with results of the monkey neurovirulence test. Therefore the only mutation occurring in Type 3 OPV which contributed to neurovirulence in monkeys was the previously described reversion at nucleotide 472. Quantitation of reversion at nucleotide 472 can be utilized for assessment of acceptability of vaccine lots, while other mutations can be used for monitoring the consistency of vaccine production. (C) 1995 Academic Press, Inc.
机译:在Sabin 3型脊髓灰质炎病毒减毒株中筛选序列异质性表明,突变在原代非洲绿猴肾(AGMK)细胞或Vero细胞连续培养10代后始终累积至显着水平。通过PCR和限制性内切酶酶切以及通过分批从Sabin原始(SO)种子病毒和RNA斑块纯化(RSO)重新获得的种子病毒在AGMK和Vero细胞中制得的商业疫苗中的商业疫苗进行突变分析,对14个新发现的突变进行了定量分析或“辉瑞”种子)。在超过一个系列的传代中可重复观察到14个突变中的9个。尽管每个仅在一组传代中观察到了5个其他突变,但是它们的含量逐渐增加到很高的百分比,这表明我们发现的所有突变都持续积累。 SO衍生的样品比RSO衍生的样品积累更多的突变,并且Vero的突变数量和积累速率高于AGMK细胞。当在37度进行传代时,大多数突变的积累速率较高,而核苷酸5832处的U→C跃迁在34度(疫苗生产所用的温度)下发生得更快。由六家制造商生产的3型口服脊髓灰质炎病毒疫苗(OPV)单池分析发现,这些新鉴定的突变在疫苗批次中仅有5种(核苷酸3956、4935、5357、5788和5832)。发现了一些突变(少于0.1%),而其他突变的含量高达1.8%。这些突变的模式是种子病毒类型和细胞底物的特征,但与结果无关。猴子神经毒性测试。因此,在3型OPV中发生的唯一导致猴子神经毒性的突变是先前描述的472位核苷酸的回复。核苷酸472位回复的定量可用于评估疫苗批次的可接受性,而其他突变可用于监测疫苗的可接受性。疫苗生产的一致性。 (C)1995 Academic Press,Inc.

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