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NK-溶素衍生抗菌肽NK-2缩短衍生物的设计原理,该衍生物对革兰氏阴性病原体具有更高活性。

Rationale for the design of shortened derivatives of the NK-lysin-derived antimicrobial peptide NK-2 with improved activity against Gram-negative pathogens.

作者信息

Andrä Jörg, Monreal Daniel, Martinez de Tejada Guillermo, Olak Claudia, Brezesinski Gerald, Gomez Susana Sanchez, Goldmann Torsten, Bartels Rainer, Brandenburg Klaus, Moriyon Ignacio

机构信息

Forschungszentrum Borstel, Leibniz-Zentrum für Medizin und Biowissenschaften, Parkallee 10, D-23845 Borstel, Germany.

出版信息

J Biol Chem. 2007 May 18;282(20):14719-28. doi: 10.1074/jbc.M608920200. Epub 2007 Mar 27.

DOI:10.1074/jbc.M608920200
PMID:17389605
Abstract

The peptide NK-2 is an effective antimicrobial agent with low hemolytic and cytotoxic activities and is thus a promising candidate for clinical applications. It comprises the alpha-helical, cationic core region of porcine NK-lysin a homolog of human granulysin and of amoebapores of pathogenic amoeba. Here we visualized the impact of NK-2 on Escherichia coli by electron microscopy and used NK-2 as a template for sequence variations to improve the peptide stability and activity and to gain insight into the structure/function relationships. We synthesized 18 new peptides and tested their activities on seven Gram-negative and one Gram-positive bacterial strains, human erythrocytes, and HeLa cells. Although all peptides appeared unordered in buffer, those active against bacteria adopted an alpha-helical conformation in membrane-mimetic environments like trifluoroethanol and negatively charged phosphatidylglycerol (PG) liposomes that mimick the cytoplasmic membrane of bacteria. This conformation was not observed in the presence of liposomes consisting of zwitterionic phosphatidylcholine (PC) typical for the human cell plasma membrane. The interaction was paralleled by intercalation of these peptides into PG liposomes as determined by FRET spectroscopy. A comparative analysis between biological activity and the calculated peptide parameters revealed that the decisive factor for a broad spectrum activity is not the peptide overall hydrophobicity or amphipathicity, but the possession of a minimal positive net charge plus a highly amphipathic anchor point of only seven amino acid residues (two helical turns).

摘要

肽NK-2是一种有效的抗菌剂,具有低溶血和细胞毒性活性,因此是临床应用的有前途的候选者。它包含猪NK-溶素的α-螺旋阳离子核心区域,猪NK-溶素是人类颗粒溶素和致病性变形虫的变形虫孔蛋白的同源物。在这里,我们通过电子显微镜观察了NK-2对大肠杆菌的影响,并将NK-2用作序列变异的模板,以提高肽的稳定性和活性,并深入了解结构/功能关系。我们合成了18种新肽,并测试了它们对7种革兰氏阴性菌和1种革兰氏阳性菌、人类红细胞和HeLa细胞的活性。尽管所有肽在缓冲液中似乎都是无序的,但那些对细菌有活性的肽在模拟膜的环境中,如三氟乙醇和模拟细菌细胞质膜的带负电荷的磷脂酰甘油(PG)脂质体中,会形成α-螺旋构象。在由人类细胞质膜典型的两性离子磷脂酰胆碱(PC)组成的脂质体存在下,未观察到这种构象。通过荧光共振能量转移光谱法测定,这些肽插入PG脂质体的过程与相互作用平行。生物活性与计算得到的肽参数之间的比较分析表明,广谱活性的决定性因素不是肽的整体疏水性或两亲性,而是拥有最小的正净电荷加上仅由七个氨基酸残基(两个螺旋圈)组成的高度两亲性锚点。

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