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螺旋稳定性赋予螺旋抗菌肽抗盐性。

Helix stability confers salt resistance upon helical antimicrobial peptides.

作者信息

Park In Yup, Cho Ju Hyun, Kim Key Sun, Kim Yun-Bae, Kim Mi Sun, Kim Sun Chang

机构信息

Department of Biological Sciences, Korea Advanced Institute of Science and Technology, Taejon 305-701, Korea.

出版信息

J Biol Chem. 2004 Apr 2;279(14):13896-901. doi: 10.1074/jbc.M311418200. Epub 2004 Jan 12.

DOI:10.1074/jbc.M311418200
PMID:14718539
Abstract

Salt sensitivity of antimicrobial peptides poses a major obstacle in their development as novel antibiotics. Here we report the use of helix-capping motifs to confer salt resistance upon helical antimicrobial peptides. The helical content of the template peptide RLLR was almost completely destroyed at salt concentrations over 200 mm NaCl, leading to a 8-32-fold decrease in antimicrobial activity. However, the introduction of helix-capping motifs at the helix termini resulted in a structurally stable peptide, which retained membrane-permeabilizing and antimicrobial activities upon exposure to salt. Furthermore, the peptide with helix-capping motifs directly inhibited the in vivo growth of Streptococcus pyogenes, which causes localized fasciitis in mice, and prevented the necrosis of the epidermis, dermis, and subcutaneous muscle layers. Results indicate that the adoption of helix-capping motifs into salt-sensitive antimicrobial peptides provides the necessary structural stability for the peptides to permeabilize cell membranes and cause cell death at physiological salt concentrations.

摘要

抗菌肽的盐敏感性是其作为新型抗生素开发过程中的一个主要障碍。在此,我们报告了利用螺旋封端基序赋予螺旋抗菌肽抗盐性。模板肽RLLR在NaCl浓度超过200 mM时,其螺旋含量几乎完全被破坏,导致抗菌活性降低8至32倍。然而,在螺旋末端引入螺旋封端基序可产生结构稳定的肽,该肽在暴露于盐环境时仍保留膜通透和抗菌活性。此外,带有螺旋封端基序的肽直接抑制了化脓性链球菌在体内的生长,该菌可在小鼠中引起局部筋膜炎,并防止了表皮、真皮和皮下肌肉层的坏死。结果表明,将螺旋封端基序应用于盐敏感抗菌肽可为肽在生理盐浓度下通透细胞膜并导致细胞死亡提供必要的结构稳定性。

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