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Fusion to an albumin-binding domain with a high affinity for albumin extends the circulatory half-life and enhances the in vivo antitumor effects of human TRAIL.

J Control Release.. 2016-04; 
Li R,Yang H,Jia D,Nie Q,Cai H,Fan Q,Wan L,Li L,Lu X.
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... The endotoxins in protein solutions were removed by using endotoxin eraser (Genscript, Nanjing, China). ... Moreover, the activities of caspases 3, 8, and 9 in apoptotic cells were detected using a specific colorimetric assay kit (Genscript, Nanjing, China). ...

摘要

Clinical applications of recombinant human tumor necrosis factor-related apoptosis-inducing ligand (hTRAIL) have been limited by their poor pharmacokinetics. Using endogenous albumin as a carrier is an attractive approach for circulatory half-life extension. Here, we produced ABD-hTRAIL and hTRAIL-ABD by fusing the albumin-binding domain (ABD) from protein G to the N- or C-terminus of hTRAIL. We found that ABD-hTRAIL bound human serum albumin (HSA) with a high affinity (0.4 ± 0.18 nM) and formed nanoparticles with an average diameter (~12 nm) above the threshold (~7 nm) of renal filtration. ABD-hTRAIL also bound mouse serum albumin (MSA); thus, its half-life was 40-50-fold greater than that of hTRAIL (14.1 ± ... More

关键词

Albumin; Albumin-binding domain; Anti-cancer drug; Cancer biotherapy; Drug delivery; Tumor necrosis factor-related apoptosis-inducing ligand