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Designing the furin-cleavable linker in recombinant immunotoxins based on Pseudomonas exotoxin A.

Bioconjug. Chem.. 2015; 
WeldonJohn E,SkarzynskiMartin,TherresJamy A,OstovitzJoshua R,ZhouHong,KreitmanRobert J,Pasta
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Gene Synthesis Mutations were generated either by Quikchange site-directed mutagenesis (Stratagene, La Jolla, CA) with primers from Lofstrand Labs Limited (Gaithersburg, MD), or by direct gene synthesis (GenScript USA Inc., Piscataway, NJ). Get A Quote

摘要

Recombinant immunotoxins (RITs) are fusion proteins that join antibodies to protein toxins for targeted cell killing. RITs armed with Pseudomonas exotoxin A (PE) are undergoing clinical trials for the treatment of cancer. The current design of PE-based RITs joins an antibody fragment to the catalytic domain of PE using a polypeptide linker that is cleaved by the protease furin. Intracellular cleavage of native PE by furin is required for cytotoxicity, yet the PE cleavage site has been shown to be a poor furin substrate. Here we describe the rational design of more efficiently cleaved furin linkers in PE-based RITs, and experiments evaluating their effects on cleavage and cytotoxicity. We found that changes ... More

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