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Synthesis and antimicrobial activity of cysteine-free coprisin nonapeptides
Authors:Jaeho Lee  Daeun Lee  Hyemin Choi  Ha Hyung Kim  Ho Kim  Jae Sam Hwang  Dong Gun Lee  Jae Il Kim
Institution:1. School of Life Sciences, Gwangju Institute of Science and Technology, Oryong-dong, Buk-gu, Gwangju 500-712, Republic of Korea;2. School of Life Sciences and Biotechnology, College of Natural Sciences, Kyungpook National University, Daehak-ro 80, Buk-gu, Daegu 702-701, Republic of Korea;3. College of Pharmacy, Chung-Ang University, Seoul, Republic of Korea;4. School of Life Sciences and Biotechnology, College of Natural Science, Daejin University, Pocheon, Gyeonggido, Republic of Korea;5. Department of Agricultural Biology, Natural Academy of Agricultural Science, RDA, Suwon 441-853, Republic of Korea
Abstract:Coprisin is a 43-mer defensin-like peptide from the dung beetle, Copris tripartitus. CopA3 (LLCIALRKK-NH2), a 9-mer peptide containing a single free cysteine residue at position 3 of its sequence, was derived from the α-helical region of coprisin and exhibits potent antibacterial and anti-inflammatory activities. The single cysteine implies a tendency for dimerization; however, it remains unknown whether this cysteine residue is indispensible for CopA3’s antimicrobial activity. To address this issue, in the present study we synthesized eight cysteine-substituted monomeric CopA3 analogs and two dimeric analogs, CopA3 (Dimer) and CopIK (Dimer), and evaluated their antimicrobial effects against bacteria and fungi, as well as their hemolytic activity toward human erythrocytes. Under physiological conditions, CopA3 (Mono) exhibits a 6/4 (monomer/dimer) molar ratio in HPLC area percent, indicating that its effects on bacterial strains likely reflect a CopA3 (Mono)/CopA3 (Dimer) mixture. We also report the identification of CopW, a new cysteine-free nonapeptide derived from CopA3 that has potent antimicrobial activity with virtually no hemolytic activity. Apparently, the cysteine residue in CopA3 is not essential for its antimicrobial function. Notably, CopW also exhibited significant synergistic activity with ampicillin and showed more potent antifungal activity than either wild-type coprisin or melittin.
Keywords:Antimicrobial activity  Antimicrobial peptide  Cysteine-free coprisin  Nonapeptide  Synergic effect
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