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Conjugation to 10 kDa linear PEG extends serum half-life and preserves the receptor-binding ability of mmTRAIL with minimal stimulation of PEG-specific antibodies

Molecular Pharmaceutics. 2016; 
Qianxue Nie, Dianong Jia, Hao Yang, Yanru Feng, Qing Fan, Qiuxiao Shi, Lin Wan, and Xiaofeng Lu
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Proteins, Expression, Isolation and Analysis The endotoxins in protein solutions were removed by using ToxinErase endotoxin removal kit combined with ToxinSensor chromogenic LAL Endotoxin Assay Kit (Genscript, Nanjing, China). Get A Quote

摘要

The poor in vivo potencies of most therapeutic proteins might be attributed to their short serum half-lives. PEGylation is a well-established method and has been clinically proven to improve pharmacokinetics. mmTRAIL exhibited supercytotoxicity in a variety of tumor cells, but its serum half-life was less than 10 min in mice. Here, mmTRAIL5K, mmTRAIL-10K, and mmTRAIL-20K were produced by N-terminus-specific PEGylation of mmTRAIL with 5, 10, or 20 kDa mPEG, respectively. The particle sizes of mmTRAIL5K, mmTRAIL-10K, and mmTRAIL-20K were 9.09 ± 2.76, 12.62 ± 4.05, and 15.68 ± 4.95 nm, which were higher than the threshold (∼7 nm) of renal clearance. Accordingly, mmTRAIL5K exhibited a serum half-life of 30 mi... More

关键词

serum half-life, PEGylation, anti-PEG antibody, cancer targeted therapy, tumor necrosis factor-related apoptosis-inducing ligand