Impact of altered endogenous IgG on unspecific mAb clearance.

J Pharmacokinet Pharmacodyn

Institute of Mathematics, Universität Potsdam, Karl-Liebknecht-Str. 24-25, 14476, Potsdam, Golm, Germany.

Published: August 2017

AI Article Synopsis

  • Immunodeficient mice serve as important models for assessing the effectiveness of monoclonal antibodies (mAbs), particularly regarding their pharmacokinetics (PK).
  • Binding to the neonatal Fc receptor (FcRn) plays a critical role in protecting these antibodies from elimination, but reduced levels of endogenous IgG in these mice complicate the understanding of this mechanism and its impact on mAb clearance.
  • By employing a pharmacokinetic modeling approach, the study investigates how altered IgG concentrations in immunodeficient mice influence unspecific mAb clearance, providing valuable insights for predicting mAb PK in clinical scenarios, especially for immunosuppressed cancer patients.

Article Abstract

Immunodeficient mice are crucial models to evaluate the efficacy of monoclonal antibodies (mAbs). When studying mAb pharmacokinetics (PK), protection from elimination by binding to the neonatal Fc receptor (FcRn) is known to be a major process influencing the unspecific clearance of endogenous and therapeutic IgG. The concentration of endogenous IgG in immunodeficient mice, however is reduced, and this effect on the FcRn protection mechanism and subsequently on unspecific mAb clearance is unknown, yet of great importance for the interpretation of mAb PK data. We used a PBPK modelling approach to elucidate the influence of altered endogenous IgG concentrations on unspecific mAb clearance. To this end, we used PK data in immunodeficient mice, i.e. nude and severe combined immunodeficiency mice. To avoid impact of target-mediated clearance processes, we focussed on mAbs without affinity to a target antigen in these mice. In addition, intravenous immunoglobulin (IVIG) data of immunocompetent mice was used to study the impact of increased total IgG concentrations on unspecific therapeutic antibody clearance. The unspecific clearance is linear, whenever therapeutic IgG concentrations, i.e. mAb and IVIG concentrations are lower than FcRn; it can be non-linear if therapeutic IgG concentrations are larger than FcRn and endogenous IgG concentrations (e.g., under IVIG therapy). Unspecific mAb clearance of immunodeficient mice is effectively linear (under mAb doses as typically used in human). Studying the impact of reduced endogenous IgG concentrations on unspecific mAb clearance is of great relevance for the extrapolation to clinical species, e.g., when predicting mAb PK in immunosuppressed cancer patients.

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http://dx.doi.org/10.1007/s10928-017-9524-2DOI Listing

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