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赖氨酸到精氨酸取代对阳离子订书肽抗菌活性的影响。

Effects of lysine-to-arginine substitution on antimicrobial activity of cationic stapled heptapeptides.

机构信息

College of Pharmacy, Dongguk University, Seoul, 100-715, Korea.

College of Pharmacy, Seoul National University, Seoul, 151-742, Korea.

出版信息

Arch Pharm Res. 2018 Nov;41(11):1092-1097. doi: 10.1007/s12272-018-1084-5. Epub 2018 Oct 25.

Abstract

We previously reported a series of amphipathic helices of stapled heptapeptides as membrane-lytic antimicrobial peptides. These peptides possess three lysine residues as the sole cationic amino acid residues in their hydrophilic face of the helix. Lysine-to-arginine substitution is often shown to increase antimicrobial activity of many natural AMPs due to the more favorable interactions of guanidinium moiety of arginine with membranes. In an effort to further improve the pharmacological properties of our novel AMP series, we here examined the impact of lysine-to-arginine substitution on their structures and antimicrobial and hemolytic activities. Our results indicate that the lysine-to-arginine substitution does not always guarantee enhancement in the antimicrobial potency of AMPs. Instead, we observed varied potency and selectivity depending on the number of substitutions and the positions substituted. Our results imply that, in the given helical scaffold stabilized by a hydrocarbon staple, antimicrobial potency and selectivity are influenced by a complex effect of various structural and chemical changes accompanied by lysine-to-arginine substitution rather than solely by the type of cationic residue. These data show potential for use in our scaffold-assisted development of short, selective, and metabolically stable AMPs.

摘要

我们之前报道了一系列作为膜溶解抗菌肽的订书肽七肽的两亲性螺旋。这些肽在其亲水螺旋面上只含有三个赖氨酸残基作为唯一的阳离子氨基酸残基。由于精氨酸的胍基部分与膜的相互作用更有利,赖氨酸到精氨酸的取代通常会增加许多天然 AMP 的抗菌活性。为了进一步改善我们新型 AMP 系列的药理学特性,我们在此研究了赖氨酸到精氨酸取代对它们的结构以及抗菌和溶血活性的影响。我们的结果表明,赖氨酸到精氨酸的取代并不总是保证 AMP 的抗菌效力增强。相反,我们观察到根据取代的数量和位置,效力和选择性有所不同。我们的结果表明,在由碳氢化合物订书钉稳定的给定螺旋支架中,抗菌效力和选择性受到赖氨酸到精氨酸取代伴随的各种结构和化学变化的复杂影响,而不仅仅是由阳离子残基的类型决定。这些数据显示了在我们的支架辅助开发短、选择性和代谢稳定的 AMP 方面的应用潜力。

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