Surrogate potency assays: Comparison of binding profiles complements dose response curves for unambiguous assessment of relative potencies
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...
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| Series: | Journal of Pharmaceutical Analysis |
| Online Access: | http://www.sciencedirect.com/science/article/pii/S2095177917301417 |
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doaj-a8e5298b70e04df8bfe3027352d96a1f2021-04-02T06:19:17ZengElsevierJournal of Pharmaceutical Analysis2095-17792018-04-0182138146Surrogate potency assays: Comparison of binding profiles complements dose response curves for unambiguous assessment of relative potenciesRobert Karlsson0Veronica Fridh1Åsa Frostell2Purification and Analysis, GE Healthcare Life Sciences, Uppsala, SwedenPurification and Analysis, GE Healthcare Life Sciences, Uppsala, SwedenCorresponding author.; Purification and Analysis, GE Healthcare Life Sciences, Uppsala, SwedenSurface 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. Keywords: Surface plasmon resonance, EC50, Sensorgram comparison, Calibration free concentration analysis, Surrogate potency assay, TNF-αhttp://www.sciencedirect.com/science/article/pii/S2095177917301417 |
| collection |
DOAJ |
| language |
English |
| format |
Article |
| sources |
DOAJ |
| author |
Robert Karlsson Veronica Fridh Åsa Frostell |
| spellingShingle |
Robert Karlsson Veronica Fridh Åsa Frostell Surrogate potency assays: Comparison of binding profiles complements dose response curves for unambiguous assessment of relative potencies Journal of Pharmaceutical Analysis |
| author_facet |
Robert Karlsson Veronica Fridh Åsa Frostell |
| author_sort |
Robert Karlsson |
| title |
Surrogate potency assays: Comparison of binding profiles complements dose response curves for unambiguous assessment of relative potencies |
| title_short |
Surrogate potency assays: Comparison of binding profiles complements dose response curves for unambiguous assessment of relative potencies |
| title_full |
Surrogate potency assays: Comparison of binding profiles complements dose response curves for unambiguous assessment of relative potencies |
| title_fullStr |
Surrogate potency assays: Comparison of binding profiles complements dose response curves for unambiguous assessment of relative potencies |
| title_full_unstemmed |
Surrogate potency assays: Comparison of binding profiles complements dose response curves for unambiguous assessment of relative potencies |
| title_sort |
surrogate potency assays: comparison of binding profiles complements dose response curves for unambiguous assessment of relative potencies |
| publisher |
Elsevier |
| series |
Journal of Pharmaceutical Analysis |
| issn |
2095-1779 |
| publishDate |
2018-04-01 |
| description |
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. Keywords: Surface plasmon resonance, EC50, Sensorgram comparison, Calibration free concentration analysis, Surrogate potency assay, TNF-α |
| url |
http://www.sciencedirect.com/science/article/pii/S2095177917301417 |
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