1. Potential Sources of Inter-Subject Variability in Monoclonal Antibody Pharmacokinetics.
- Author
-
Gill, Katherine, Machavaram, Krishna, Rose, Rachel, Chetty, Manoranjenni, Gill, Katherine L, Machavaram, Krishna K, and Rose, Rachel H
- Subjects
THERAPEUTIC use of monoclonal antibodies ,PHARMACODYNAMICS ,PHARMACOKINETICS ,DRUG toxicity ,COMORBIDITY ,GENETIC polymorphisms ,DRUG dosage ,AGE distribution ,ANTHROPOMETRY ,BIOLOGICAL models ,CELL receptors ,DRUG interactions ,DOSE-effect relationship in pharmacology ,ETHNIC groups ,HISTOCOMPATIBILITY antigens ,LYMPHATICS ,MONOCLONAL antibodies ,SEX distribution ,SYSTEMATIC reviews ,SEVERITY of illness index - Abstract
Understanding inter-subject variability in drug pharmacokinetics and pharmacodynamics is important to ensure that all patients attain suitable drug exposure to achieve efficacy and avoid toxicity. Inter-subject variability in the pharmacokinetics of therapeutic monoclonal antibodies (mAbs) is generally moderate to high; however, the factors responsible for the high inter-subject variability have not been comprehensively reviewed. In this review, the extent of inter-subject variability for mAb pharmacokinetics is presented and potential factors contributing to this variability are explored and summarised. Disease status, age, sex, ethnicity, body size, genetic polymorphisms, concomitant medication, co-morbidities, immune status and multiple other patient-specific details have been considered. The inter-subject variability for mAb pharmacokinetics most likely depends on the complex interplay of multiple factors. However, studies aimed at investigating the reasons for the inter-subject variability are sparse. Population pharmacokinetic models and physiologically based pharmacokinetic models are useful tools to identify important covariates, aiding in the understanding of factors contributing to inter-subject variability. Further understanding of inter-subject variability in pharmacokinetics should aid in development of dosing regimens that are more appropriate. [ABSTRACT FROM AUTHOR]
- Published
- 2016
- Full Text
- View/download PDF