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In silico design of a novel chimeric shigella IpaB fused to C terminal of clostridium perfringens enterotoxin as a vaccine candidate.

Bioengineered. 2018; 
ArabshahiSina,Nayeri FasaeiBahar,DerakhshandehAbdollah,NovinroozA
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Codon Optimization The codon adaptation indices (CAIs) of the codon-optimized and nonoptimized recombinant genes were analyzed by both the OPTIMIZER and GenScript rare codon analysis tools. Get A Quote

摘要

This study aimed to design a novel chimeric protein in silico to serve as a serotype-independent vaccine candidate against Shigella. The chimera contains amino acid residues 240-460 of Shigella invasion plasmid antigen B (IpaB) and the C-terminus of Clostridium perfringens enterotoxin (C-CPE). Amino acid sequences of 537 peptide linkers were obtained from two protein linker databases. 3D structures of IpaB-CPE, IpaB-CPE, IpaB-CPE and 537 newly designed IpaB-linker-CPE constructs with varying linker regions were predicted. These predicted 3D structures were merged with the 3D structures of native IpaB, CPE, CPE and CPE to select the structure most similar to native IpaB and C-CPE. Several in silico tools... More

關(guān)鍵詞

CPE,Chimeric protein,IpaB,Shigella,Vaccine candi
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