Antimicrobial activity and stability of the d-amino acid substituted derivatives of antimicrobial peptide polybia-MPI

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作者
Yanyan Zhao
Min Zhang
Shuai Qiu
Jiayi Wang
Jinxiu Peng
Ping Zhao
Ranran Zhu
Hailin Wang
Yuan Li
Kairong Wang
Wenjin Yan
Rui Wang
机构
[1] Lanzhou University,Key Laboratory of Preclinical Study for New Drugs of Gansu Province, School of Basic Medical Sciences
[2] The People’s Hospital in Gansu Province,undefined
来源
AMB Express | / 6卷
关键词
Antimicrobial peptide; -MPI; Stability; -Amino acid substitution;
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摘要
Antimicrobial peptide has the potential to be developed as new kind of antimicrobial agents with novel action mechanism. However, the susceptibility to protease is a drawback for potential peptides to be clinical used. d-amino acid substitution can be one way to increase the proteolytic stability of peptides. In the present study, we synthesized the d-lysines substituted analog (d-lys-MPI) and the d-enantiomer of polybia-MPI (D-MPI) to improve the proteolytic resistance of polybia-MPI. Our results showed that, the stability of its d-amino acid partially substituted analog d-lys-MPI was increased. However, it lost antimicrobial activity at the tested concentration with the loss of α-helix content. As shown in the CD spectra, after substitution, the spectra of D-MPI is symmetrical to MPI, indicated it turned into left hand α-helical conformation. Excitingly, the stability of D-MPI toward the tested protease was improved greatly. Notably, the antimicrobial activity of D-MPI was comparable to its L-counterpart MPI, even improved. In addition, the hemolytic activity of D-MPI was lowered. This also indicated that the action target of antimicrobial peptide polybia-MPI was not chiral specific. So, D-MPI may offer a therapeutic strategy to defend the infection of microbes, considering its stability to protease and relatively lower cytotoxicity to human erythrocytes.
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