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疏水作用控制从头设计的抗菌肽的生物活性和细胞毒性。

Hydrophobic Control of the Bioactivity and Cytotoxicity of de Novo-Designed Antimicrobial Peptides.

出版信息

ACS Appl Mater Interfaces. 2019 Sep 25;11(38):34609-34620. doi: 10.1021/acsami.9b10028. Epub 2019 Sep 10.

Abstract

Antimicrobial peptides (AMPs) can target bacterial membranes and kill bacteria through membrane structural damage and cytoplasmic leakage. A group of surfactant-like cationic AMPs was developed from substitutions to selective amino acids in the general formula of G(IIKK)I-NH, (called G, a de novo AMP), to explore the correlation between AMP hydrophobicity and bioactivity. A threshold surface pressure over 12 mN/m was required to cause measurable antimicrobial activity and this corresponded to a critical AMP concentration. Greater surface activity exhibited stronger antimicrobial activity but had the drawback of worsening hemolytic activity. Small unilamellar vesicles (SUVs) with specific lipid compositions were used to model bacterial and host mammalian cell membranes by mimicking the main structural determinants of the charge and composition. Leakage from the SUVs of encapsulated carboxyfluorescein measured by fluorescence spectroscopy indicated a negative correlation between hydrophobicity and model membrane selectivity, consistent with measurements of the zeta potential that demonstrated the extent of AMP binding onto model SUV lipid bilayers. Experiments with model lipid membranes thus explained the trend of minimum inhibitory concentrations and selectivity measured from real cell systems and demonstrated the dominant influence of hydrophobicity. This work provides useful guidance for the improvement of the potency of AMPs via structural design, whilst taking due consideration of cytotoxicity.

摘要

抗菌肽 (AMPs) 可以通过破坏细菌膜结构和细胞质渗漏来靶向细菌膜并杀死细菌。一组表面活性剂样阳离子 AMP 是通过在 G(IIKK)I-NH 的一般公式中对选择性氨基酸进行取代而开发的(称为 G,一种从头合成的 AMP),以探索 AMP 疏水性和生物活性之间的相关性。需要超过 12 mN/m 的临界表面压力才能引起可测量的抗菌活性,这对应于临界 AMP 浓度。更高的表面活性表现出更强的抗菌活性,但存在溶血活性恶化的缺点。具有特定脂质组成的小单层囊泡 (SUV) 通过模拟电荷和组成的主要结构决定因素来模拟细菌和宿主哺乳动物细胞膜。通过荧光光谱法测量包封的羧基荧光素从 SUV 中的泄漏表明疏水性与模型膜选择性之间存在负相关,与测量证明 AMP 结合到模型 SUV 脂质双层的程度的 ζ 电位一致。因此,与真实细胞系统测量的最小抑菌浓度和选择性的实验表明,疏水性具有主导影响。这项工作为通过结构设计提高 AMP 的效力提供了有用的指导,同时充分考虑细胞毒性。

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