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Pharmacokinetics of protein and peptide conjugates
Institution:1. Department of Gastrointestinal Oncology, H. Lee Moffitt Cancer Center & Research Institute, FOB-2, Tampa, FL 334612, USA;2. Biotherapeutics Discovery, Takeda Pharmaceuticals International, Co 35 Landsdowne Street, Cambridge, MA 02139, USA;3. Clinical Research, Takeda Pharmaceuticals International, Oncology Co 35 Landsdowne Street, Cambridge, MA 02139, USA
Abstract:Protein and peptide conjugates have become an important component of therapeutic and diagnostic medicine. These conjugates are primarily designed to improve pharmacokinetics (PK) of those therapeutic or imaging agents, which do not possess optimal disposition characteristics. In this review we have summarized preclinical and clinical PK of diverse protein and peptide conjugates, and have showcased how different conjugation approaches are used to obtain the desired PK. We have classified the conjugates into peptide conjugates, non-targeted protein conjugates, and targeted protein conjugates, and have highlighted diagnostic and therapeutic applications of these conjugates. In general, peptide conjugates demonstrate very short half-life and rapid renal elimination, and they are mainly designed to achieve high contrast ratio for imaging agents or to deliver therapeutic agents at sites not reachable by bulky or non-targeted proteins. Conjugates made from non-targeted proteins like albumin are designed to increase the half-life of rapidly eliminating therapeutic or imaging agents, and improve their delivery to tissues like solid tumors and inflamed joints. Targeted protein conjugates are mainly developed from antibodies, antibody derivatives, or endogenous proteins, and they are designed to improve the contrast ratio of imaging agents or therapeutic index of therapeutic agents, by enhancing their delivery to the site-of-action.
Keywords:Pharmacokinetics  Peptide-drug conjugate  Antibody-drug conjugate  PEGylation  Radioimmunoconjugate  Immunotoxin  Albumin conjugates
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