Bypassing nonparallelism of a monoclonal antibody ligand-binding assay by employment of alternative assay formats
Determination of concentration-time profiles in cynomolgus monkeys of a therapeutic monoclonal antibody against a soluble target revealed a substantial discrepancy between a generic anti-human IgG capture/detection and target bridging assay with the target bridging assay leading to dose- and time-de...
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Veröffentlicht in: | Bioanalysis 2016-12, Vol.8 (24), p.2581-2593 |
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Format: | Artikel |
Sprache: | eng |
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Zusammenfassung: | Determination of concentration-time profiles in cynomolgus monkeys of a therapeutic monoclonal antibody against a soluble target revealed a substantial discrepancy between a generic anti-human IgG capture/detection and target bridging assay with the target bridging assay leading to dose- and time-dependent underquantification of drug concentrations, lack of parallelism and subsequently different pharmacokinetic parameters. In contrast, plasma levels derived from a target capture and an anti-idiotypic antibody bridging assay were in close concordance with the generic assay and demonstrated parallelism with high precision across several dilutions. The results provide a practical attempt to overcome nonparallelism by employing alternative assay formats utilizing tailored assay reagent combinations in order to obtain unbiased pharmacokinetic data. |
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ISSN: | 1757-6180 1757-6199 |
DOI: | 10.4155/bio-2016-0076 |