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Surrogate potency assays: Comparison of binding profiles complements dose response curves for unambiguous assessment of relative potencies

机译:替代效价测定:结合谱的比较补充了剂量响应曲线可明确评估相对效价

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摘要

Surface plasmon resonance (SPR) systems are widely used for detailed characterization of antibody activities including antigen and Fc-receptor binding. During the later stages of development, where the focus is to ensure that established critical quality attributes (CQAs) are maintained during cell culture, purification and formulation processes, analysis is simplified, and relative potencies are often determined. Here, simulation of binding data revealed that relative potency values, determined via parallel line analysis (PLA) and half maximal effective concentration (EC50) analysis accurately reflect changes in active concentration only if binding kinetics remain unchanged. Changes in the association rate constant shifted dose response curves, and therefore relative potencies, in the same way as changes in analyte concentration do. However, for interactions characterized by stable binding, changes in the dissociation rate constant did not result in any shift, suggesting that this type of change may go unnoticed in the dose response curve. Thus, EC50 and PLA analyses of dose response curves obtained with an anti-TNF-α antibody were complemented with the Biacore functionality for sensorgram comparison analysis, whereby changes in antigen and Fc-receptor binding profiles could be detected. Next, analysis of temperature stressed TNF-α antibody revealed that calibration free concentration analysis (CFCA) data correlated perfectly with relative potency values. Together, these results demonstrate that combinations of SPR based dose response curves, sensorgram comparison and CFCA can be used to strengthen the confidence in relative potency assessments, and suggest that SPR can potentially be used as a surrogate potency assay in the quality control of biotherapeutic medicines.
机译:表面等离子体共振(SPR)系统广泛用于抗体活性的详细表征,包括抗原和Fc受体结合。在开发的后期阶段,重点是确保在细胞培养,纯化和配制过程中保持已建立的关键质量属性(CQA),简化了分析并经常确定相对效价。在这里,结合数据的模拟显示,只有在结合动力学保持不变的情况下,通过平行线分析(PLA)和半数最大有效浓度(EC50)分析确定的相对效价值才能准确反映活性浓度的变化。缔合速率常数位移剂量响应曲线的变化,以及因此相对效力的变化,与分析物浓度的变化相同。但是,对于以稳定结合为特征的相互作用,解离速率常数的变化不会导致任何变化,这表明这种类型的变化可能不会在剂量反应曲线中引起注意。因此,用抗TNF-α抗体获得的剂量反应曲线的EC50和PLA分析与Biacore功能互补,用于传感图比较分析,从而可以检测到抗原和Fc受体结合概况的变化。接下来,对温度胁迫的TNF-α抗体的分析表明,无标定浓度分析(CFCA)数据与相对效价值完美相关。总之,这些结果表明,基于SPR的剂量反应曲线,传感图比较和CFCA的组合可用于增强相对效价评估的可信度,并表明SPR可用作生物治疗药物质量控制中的替代效价测定法。 。

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