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Linear bactenecin analogs with cell selectivity and anti‐endotoxic activity
Authors:Yong Hai Nan  Binu Jacob  Yangmee Kim  Song Yub Shin
Affiliation:1. Department of Bio‐Materials, Graduate School, Chosun University, , Gwangju, 501‐759 Korea;2. Department of Bioscience and Biotechnology, Bio/Molecular Informatics Center, Konkuk University, , Seoul, 143‐701 Korea;3. Department of Cellular & Molecular Medicine, School of Medicine, Chosun University, , Gwangju, 501‐759 Korea
Abstract:Bactenecin (Bac) is a 12‐residue disulfide‐linked antimicrobial peptide isolated from the granules of bovine neutrophils. In this study, to develop novel linear Bac analogs with cell selectivity and anti‐endotoxic activity, we designed and synthesized a series of linear Bac analogs with amino acid substitution in Cys3,11 and/or Val6,7 of Bac. Among Bac analogs, some analogs (Bac‐W, Bac‐KW, Bac‐L, Bac‐KL, Bac‐LW, and Bac‐KLW) with higher hydrophobicity showed the amalgamated property of cell selectivity and anti‐endotoxic activity. Furthermore, Bac‐W, Bac‐KW, Bac‐LW, and Bac‐KLW showed serum stability comparable with that of disulfide‐bonded Bac. Therefore, these Bac analogs (Bac‐W, Bac‐KW, Bac‐LW, and Bac‐KLW) can serve as promising antibiotics for the development of therapeutic agents for treatment against endotoxic shock and bacterial infection. In addition, our results suggest that a little increase in hydrophobicity may be responsible for the decreased cell selectivity of the multiple Arg‐containing peptides (Bac‐W, Bac‐L, and Bac‐LW) over the multiple Lys‐containing peptides (Bac‐KW, Bac‐KL, and Bac‐KLW). Copyright © 2012 European Peptide Society and John Wiley & Sons, Ltd.
Keywords:linear bactenecin analogs  cell selectivity  anti‐endotoxin activity  serum stability
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