VIII International Symposium on Chemistry and Pharmaceutical Sciences

CogiTx1 is a defensin-like subtilisin inhibitor isolated from the sea anemone C. gigantea and its in-depth functional characterization needs to be completed. Since the purification from the natural source has a very low yield, a source of pure and well-folded protein is needed. Therefore, the aim of this work was to obtain two recombinant variants of CogiTx1. To achieve this goal, the sequence of CogiTx1 variants, optimized for expression in Escherichia coli, including a TEV protease site, were inserted in the plasmid pET32Aa (pET32a/CogiTx1_R and pET32a/CogiTX1_S) and expressed in SHuffle E. coli cells as fusion proteins Trx-TEV-CogiTX1_R/S. CogiTx1_S and CogiTx1_R are well-folded peptides with 4970 and 5190 Da respectively and both molecules present the expected amino acid sequence. CogiTx1_S is active against subtilisin, porcine pancreatic elastase, proteinase K and Stenothophomonas maltophilia protease 1 (rStmPr1). However, CogiTx1_R is not active against any of the enzymes evaluated, result that could be due to the presence of two extra residues –GR at the C-terminal when compared with CogiTx1_S (sequence of the natural protein). In conclusion, the expression in E. coli of CogiTx1 variants was successful and the results suggest that the modification observed in the natural protein is important for the activity of CogiTx1