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Estimating viral titres in solutions with low viral loads.

机译:在低病毒载量的溶液中估算病毒滴度。

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An important consideration in the manufacture of products derived from animal or human sources is the virus reduction capacity of the manufacturing process as estimated using validated bench-scale models of relevant manufacturing steps. In these studies, manufacturing process intermediates are spiked with virus and processed using the bench-scale model and the resulting viral titres of input and output samples are typically determined using cell-based infectivity assays. In these assays, the Spearman-Karber (SK) method is commonly used to estimate titres when there is one or more positive observation (i.e., the presence of any viral cytopathic effect). The SK method is most accurate when the proportion of positive observations ranges from <0.1 to >0.9 across dilutions but can be biased otherwise. Maximum likelihood (ML) based on a single-hit Poisson model is an alternative widely used estimation method. We compared SK with ML and found the methods to have similar properties except for situations in which the concentration of virus is low but measurable. In this case, the SK method produces upwardly biased estimates of titres. Based on our results, we recommend the use of either ML or SK at most virus concentrations; however, at low virus concentrations ML is preferred.
机译:在生产源自动物或人类来源的产品时,重要的考虑因素是使用相关制造步骤的经过验证的台式模型估算的制造过程中的病毒减少能力。在这些研究中,制造过程中的中间体掺有病毒,并使用台式模型进行处理,通常使用基于细胞的传染性测定法确定输入和输出样品的病毒滴度。在这些测定中,当存在一个或多个阳性观察结果(即,存在任何病毒性细胞病变作用)时,通常使用Spearman-Karber(SK)方法估算滴度。当阳性观察结果的比例在所有稀释液中的范围从<0.1到> 0.9时,SK方法是最准确的,但在其他方面可能会有偏差。基于一次命中泊松模型的最大似然(ML)是另一种广泛使用的估计方法。我们将SK与ML进行了比较,发现该方法具有相似的特性,但病毒浓度较低但可测量的情况除外。在这种情况下,SK方法会得出滴度的向上估计值。根据我们的结果,我们建议在大多数病毒浓度下使用ML或SK。但是,在低病毒浓度下,ML是首选。

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