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13个氨基酸残基的抗菌溶血肽PKLLKTFLSKWIG的添加和缺失类似物:结构偏好、模拟膜结合及生物活性

Addition and omission analogs of the 13-residue antibacterial and hemolytic peptide PKLLKTFLSKWIG: structural preferences, model membrane binding and biological activities.

作者信息

Bikshapathy E, Sitaram N, Nagaraj R

机构信息

Centre for Cellular and Molecular Biology, Hyderabad, India.

出版信息

J Pept Res. 1999 Jan;53(1):47-55. doi: 10.1111/j.1399-3011.1999.tb01616.x.

DOI:10.1111/j.1399-3011.1999.tb01616.x
PMID:10195441
Abstract

The consequences of selective addition or deletion of polar amino acids in a 13-residue antibacterial peptide PKLLKTFLSKWIG on structure, membrane binding and biological activities have been investigated. The variants generated are (a) S and T residues replaced by K, (b) S and T residues deleted individually and together, (c) introduction of two additional K and (d) deletion of L and L with T. In the aqueous environment all the peptides were unordered. In trifluoroethanol, the spectra of peptides belonging to groups (a-c) suggest distorted helical conformation. Peptides in group (d) appear to adopt beta-sheet conformation. The peptides bind to zwitterionic and negatively charged lipid vesicles, although to different extents. With the exception of peptides in group (d), all the other peptides exhibited comparable antibacterial activity against Escherichia coli and Staphylococcus aureus. However, the changes made in the peptides in groups (a-c) resulted in reduction of hemolytic activity compared to the parent peptide. Extent of binding to lipid vesicles composed of phosphatidylcholine and cholesterol appears to correlate with hemolytic activity. It appears that polar and charged residues play a major role in modulating the biological activities of the 13-residue peptide PKLLKTFLSKWIG. The 11-residue peptide-like PKLLKFLKWIG has selective antibacterial activity. Thus, by judicious engineering it should be possible to generate short peptides with selective antibacterial activity.

摘要

研究了在13个氨基酸残基的抗菌肽PKLLKTFLSKWIG中选择性添加或缺失极性氨基酸对其结构、膜结合及生物活性的影响。所产生的变体包括:(a) 将S和T残基替换为K;(b) 分别或同时缺失S和T残基;(c) 额外引入两个K;(d) 缺失L以及L与T一起缺失。在水性环境中,所有肽均无序。在三氟乙醇中,属于(a - c)组的肽的光谱表明其螺旋构象扭曲。(d)组的肽似乎呈现β-折叠构象。这些肽与两性离子和带负电荷的脂质囊泡结合,尽管结合程度不同。除了(d)组的肽之外,所有其他肽对大肠杆菌和金黄色葡萄球菌均表现出相当的抗菌活性。然而,与亲本肽相比,(a - c)组肽的变化导致溶血活性降低。与由磷脂酰胆碱和胆固醇组成的脂质囊泡的结合程度似乎与溶血活性相关。看来极性和带电荷的残基在调节13个氨基酸残基的肽PKLLKTFLSKWIG的生物活性中起主要作用。11个氨基酸残基的类似肽PKLLKFLKWIG具有选择性抗菌活性。因此,通过合理设计,应该有可能产生具有选择性抗菌活性的短肽。

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