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Understanding Inter-Individual Variability in Monoclonal Antibody Disposition

机译:了解单克隆抗体处置中的个体差异

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摘要

Monoclonal antibodies (mAbs) are currently the largest and most dominant class of therapeutic proteins. Inter-individual variability has been observed for several mAbs; however, an understanding of the underlying mechanisms and factors contributing to inter-subject differences in mAb disposition is still lacking. In this review, we analyze the mechanisms of antibody disposition and the putative mechanistic determinants of inter-individual variability. Results from in vitro, preclinical, and clinical studies were reviewed evaluate the role of the neonatal Fc receptor and Fc gamma receptors (expression and polymorphism), target properties (expression, shedding, turnover, internalization, heterogeneity, polymorphism), and the influence of anti-drug antibodies. Particular attention is given to the influence of co-administered drugs and disease, and to the physiological relevance of covariates identified by population pharmacokinetic modeling, as determinants of variability in mAb pharmacokinetics.
机译:单克隆抗体(mAb)是目前治疗蛋白质中最大和最主要的类别。已观察到几种mAb的个体间差异;但是,仍然缺乏对导致mAb处置对象间差异的潜在机制和因素的了解。在这篇综述中,我们分析了抗体配置的机制以及个体间变异性的推定机制决定因素。回顾了体外,临床前和临床研究的结果,评估了新生儿Fc受体和Fcγ受体的作用(表达和多态性),靶标属性(表达,脱落,周转率,内在化,异质性,多态性)以及抗药物抗体。特别注意共同给药的药物和疾病的影响,以及通过群体药代动力学模型鉴定的协变量的生理相关性,这些变量是mAb药代动力学变异性的决定因素。

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