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A combinatorial strategy for HRV 3C protease engineering to achieve the N-terminal free cleavage

Int J Biol Macromol. 2024-03; 
Meng Mei, Xian Fan, Yu Zhou, Faying Zhang, Guimin Zhang, Li Yi
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Gene Synthesis … These findings underscore the potential of TMSB10 UTR as a strategic component in mRNA … The plasmids were synthesized by GenScript (Nanjing, China) and cloned into pUC57 … Get A Quote

摘要

Human rhinovirus 3C protease (HRV 3CP) has a high specificity against the substrate of LEVLFQ↓G at P1' site, which plays an important role in biotechnology and academia as a fusion tag removal tool. However, a non-ignorable limitation is that an extra residue of Gly would remain at the N terminus of the recombinant target protein after cleavage with HRV 3CP, thus potentially causing protein mis-functionality or immunogenicity. Here, we developed a combinatorial strategy by integrating structure-guided library design and high-throughput screening of eYESS approach for HRV 3CP engineering to expand its P1' specificity. Finally, a C3 variant was obtained, exhibiting a broad substrate P1' specificity to recognize... More

關鍵詞

Directed evolution, HRV 3C protease, Substrate specificity
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