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首页> 外文期刊>Biotechnology Progress >Challenges with Afucosylation Content in Antibody-based Drugs: Guidance Provided by Mathematical Modeling
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Challenges with Afucosylation Content in Antibody-based Drugs: Guidance Provided by Mathematical Modeling

机译:基于抗体的药物中岩藻糖基化含量的挑战:数学建模提供的指导

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The theory of competitive ligand-receptor binding has been used to analyze the effect of afucosylation-based antibody heterogeneity on Fc-Fc gamma RIIIa ligand-receptor binding activity. In vitro activity is found to represent a linear combination of the component antibody activities, weighted by the relative concentrations of the different afucosylated antibody forms. An analysis of ELISA binding activity data has allowed for the dissection of the activity contributions of the different afucosylated antibodies, revealing that the heterogeneous afucosylated antibody exhibits greater activity, on a per mole basis, when compared to the homogeneous afucosylated antibody. The ratio of the afucosylated antibody equilibrium dissociation constants is computed to be K-AF/K-A approximate to 0.6-0.9, where K-AF and K-A denote the dissociation equilibrium constant of the heterogeneous and the homogeneous afucosylated antibodies, respectively. Our analysis also reveals that, in general, activity scales quadratically with the afucosylated glycan content of a sample. Linear activity-afucosylated glycan fraction correlations reported in the literature are shown to represent specific cases of this general scaling and result from oversimplifying the underlying antibody concentration distributions. The implications of our findings for drug development are also discussed. (C) 2015 American Institute of Chemical Engineers
机译:竞争性配体-受体结合的理论已用于分析基于岩藻糖基化的抗体异质性对Fc-FcγRIIIa配体-受体结合活性的影响。发现体外活性代表组分抗体活性的线性组合,由不同岩藻糖基化抗体形式的相对浓度加权。 ELISA结合活性数据的分析允许解剖不同的岩藻糖基化抗体的活性贡献,揭示与均质岩藻糖基化抗体相比,异质岩藻糖基化抗体按摩尔计表现出更高的活性。岩藻糖基化抗体平衡解离常数的比率经计算为约0.6-0.9的K-AF / K-A,其中K-AF和K-A分别表示异质岩藻糖基化抗体和均质岩藻糖基化抗体的解离平衡常数。我们的分析还显示,一般而言,活性随样品中岩藻糖基化聚糖含量的变化呈二次方关系。文献中报道的线性活性-岩藻糖基化的聚糖级分相关性表明代表了这种普遍规模的特定情况,并且是由于过度简化了潜在的抗体浓度分布而导致的。还讨论了我们的发现对药物开发的影响。 (C)2015美国化学工程师学会

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