The biodistribution of therapeutic proteins: Mechanism, implications for pharmacokinetics, and methods of evaluation

被引:24
作者
Conner, Kip P. [1 ]
Devanaboyina, Siva Charan [1 ]
Thomas, Veena A. [1 ]
Rock, Dan A. [1 ]
机构
[1] Amgen Inc, Dept Pharmacokinet & Drug Metab, 1120 Vet Blvd, San Francisco, CA 94080 USA
关键词
NEONATAL FC-RECEPTOR; BLOOD-BRAIN-BARRIER; MONOCLONAL-ANTIBODY PHARMACOKINETICS; GROWTH-FACTOR RECEPTOR; I-RELATED RECEPTOR; PEGYLATED INSULIN LISPRO; HUMAN TUMOR XENOGRAFT; HIGH-AFFINITY BINDING; ACTING BASAL INSULIN; AMYLOID-BETA PEPTIDE;
D O I
10.1016/j.pharmthera.2020.107574
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
Therapeutic proteins (TPs) are a diverse drug class that include monoclonal antibodies (mAbs), recombinantly expressed enzymes, hormones and growth factors, cytokines (e.g. chemokines, interleukins, interferons), as well as a wide range of engineered fusion scaffolds containing IgG1 Fc domain for half-life extension. As the pharmaceutical industry advances more potent and selective protein-based medicines through discovery and into the clinical stages of development, it has become widely appreciated that a comprehensive understanding of the mechanisms of TP biodistribution can aid this endeavor. This review aims to highlight the literature that has advanced our understanding of the determinants of TP biodistribution. A particular emphasis is placed on the multifaceted role of the neonatal Fc receptor (FcRn) in mAb and Fc-fusion protein disposition. In addition, characterization of the TP-target interaction at the cell-level is discussed as an essential strategy to establish pharmacokinetic-pharmacodynamic (PK/PD) relationships that may lead to more informed human dose projections during clinical development. Methods for incorporation of tissue and cell-level parameters defining these characteristics into higher-order mechanistic and semi-mechanistic PK models will also be presented. Published by Elsevier Inc.
引用
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页数:25
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