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新型乳铁蛋白抗菌肽类似物对O157:H7肠出血性大肠杆菌的设计与活性

Design and activity of novel lactoferrampin analogues against O157:H7 enterohemorrhagic Escherichia coli.

作者信息

Cruz Jenniffer, Ortiz Claudia, Guzmán Fanny, Cárdenas Constanza, Fernandez-Lafuente Roberto, Torres Rodrigo

机构信息

Grupo de Investigación en Bioquímica y Microbiología (GIBIM), Escuela de Química, Universidad Industrial de Santander, Edificio Camilo Torres 202, Bucaramanga, Colombia.

出版信息

Biopolymers. 2014 Apr;101(4):319-28. doi: 10.1002/bip.22360.

DOI:10.1002/bip.22360
PMID:23877962
Abstract

Lactoferrampin 265-284 (LFampin 265-284) is a peptide consisting of residues 265-284 of N1-domain of bovine Lactoferrin (LF). This peptide has several cationic groups in the C-terminal lobe, exhibiting an antibacterial activity against a wide range of microorganisms. However, LFampin 265-284 exhibits low antimicrobial activity against the O157:H7 enterohaemorrhagic Escherichia coli (EHEC O157:H7) when compared with Lactoferrin chimera and Lactoferricin. Here, we have designed three analogues of LFampin 265-284 based on the distribution of cationic groups, hydrophobicity, size, and sequence. Analogues were synthesized by solid phase chemistry using Fmoc methodology obtaining peptides with 95% purity. All peptides maintain the ability to adopt helical conformations (checked by circular dichroism spectra and molecular simulations). Some of these analogues exhibited a significant increase in antimicrobial activity by counting colony forming units against EHEC O157:H7 compared to native LFampin 265-284, with MIC of 10 and 40 µM for 264G-D265K and 264G-D265K/S272R, respectively. The incorporation of a GKLI sequence in the N-terminal lobe increased dramatically its antibacterial activity, an effect which has been attributed to the addition of cationic groups in the N-terminal side that may stabilize the helical conformation of the new designed peptides.

摘要

乳铁杀菌肽265 - 284(LFampin 265 - 284)是一种由牛乳铁蛋白(LF)N1结构域的265 - 284位残基组成的肽。该肽在C末端叶中有几个阳离子基团,对多种微生物具有抗菌活性。然而,与乳铁蛋白嵌合体和乳铁传递蛋白相比,LFampin 265 - 284对O157:H7肠出血性大肠杆菌(EHEC O157:H7)的抗菌活性较低。在此,我们基于阳离子基团的分布、疏水性、大小和序列设计了LFampin 265 - 284的三种类似物。使用Fmoc方法通过固相化学合成类似物,得到纯度为95%的肽。所有肽都保持了形成螺旋构象的能力(通过圆二色光谱和分子模拟检测)。与天然的LFampin 265 - 284相比,通过计算针对EHEC O157:H7的菌落形成单位,其中一些类似物的抗菌活性显著增加,264G - D265K和264G - D265K/S272R的最低抑菌浓度分别为10和40 μM。在N末端叶中引入GKLI序列显著提高了其抗菌活性,这种效应归因于在N末端一侧添加了阳离子基团,这可能稳定了新设计肽的螺旋构象。

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