Impact of lipidation site on the activity of α-helical antimicrobial peptides

IF 4.5 2区医学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY

Bioorganic Chemistry Pub Date : 2024-09-13 DOI:10.1016/j.bioorg.2024.107821

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Abstract

Antimicrobial peptides (AMPs) display advantages over traditional antibiotics due to their broad spectrum of activity against various pathogens, and may even overcome bacterial drug resistance. However, despite their potential therapeutic benefits, widespread application of AMPs is limited by their instability, sensitivity to high salt concentrations, toxicity, and immunogenicity. Lipidation is a promising strategy in overcoming these drawbacks and potential problems for drug candidates. While N-terminal lipidation is a well-studied form of acylation of biologically active peptides, fatty acylation of the lysine side chain has still been poorly explored. In this study, we examined systematic introduction of octanoic (C₈) or decanoic (C₁₀) acid into the sequences of three antimicrobial α-helical peptides, namely LL-I, LK6, and ATRA-1, by acylation of subsequent lysine residues, resulting in 17 lipopeptides. Fatty acid lengths optimal for antimicrobial activity were selected based on a previous study on the N-terminal lipidated counterparts of these peptides. Shuffling the position of the fatty acid tails in the sequences of the peptides preserved high activity against Gram-positive bacteria, increased activity against Gram-negative strains and reduced cytotoxicity, compared to the N-terminal acylated counterparts. In the case of the LL-I and LK6 conjugates, the interactions with artificial negatively charged membranes induced formation of an α-helical structure but without a direct correlation between helicity and amphipathicity. Unexpectedly, the ATRA-1 derivatives showed only a small tendency, if any, to adopt a helical structure upon binding to POPG vesicles, which may indicate a non-helical active conformation. A more detailed study of the selected analogues, namely LL-I-4C₈, LK6-7C₈, and ATRA-1-11C₁₀, provided evidence of a tendency to self-assemble into clumped and/or isolated fibrils, micelles or clusters of micelles, and proved that the lipid bilayer is the main target of action of the tested lipopeptides. In summary, the results of the present study highlight that alternative conjugation sites for lipid modification of AMPs, rather than the commonly applied N-terminal conjugation site, may improve the selectivity of action and be feasible in testing for the development of new lipid-peptide conjugates.

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脂化部位对α螺旋抗菌肽活性的影响

与传统抗生素相比，抗菌肽（AMPs）具有广谱抗各种病原体的优势，甚至可以克服细菌的耐药性。然而，尽管抗菌肽具有潜在的治疗优势，但其不稳定性、对高浓度盐的敏感性、毒性和免疫原性限制了其广泛应用。脂化是克服这些缺点和候选药物潜在问题的一种有前途的策略。虽然 N 端脂化是生物活性肽酰化的一种研究较多的形式，但对赖氨酸侧链的脂肪酰化研究还很少。在这项研究中，我们研究了在三种抗菌α-螺旋肽（即 LL-I、LK6 和 ATRA-1）的序列中系统地引入辛酸（C8）或癸酸（C10），通过对随后的赖氨酸残基进行酰化，产生了 17 种脂肽。根据之前对这些多肽 N 端脂化对应物的研究，选择了最适合抗菌活性的脂肪酸长度。与 N 端酰化的对应物相比，调整肽序列中脂肪酸尾的位置可保持对革兰氏阳性菌的高活性，提高对革兰氏阴性菌株的活性，并降低细胞毒性。就 LL-I 和 LK6 共轭物而言，与人工负电荷膜的相互作用诱导形成了一种 α 螺旋结构，但螺旋度和两性度之间并无直接关联。出乎意料的是，ATRA-1 衍生物在与 POPG 囊泡结合时，即使有螺旋结构，也只表现出很小的倾向，这可能表明其具有非螺旋活性构象。对所选类似物（即 LL-I-4C8、LK6-7C8 和 ATRA-1-11C10）进行的更详细研究证明，这些类似物倾向于自组装成团块状和/或孤立的纤维、胶束或胶束簇，并证明脂质双分子层是所测试脂肽的主要作用目标。总之，本研究的结果突出表明，脂质修饰 AMPs 的替代连接位点，而不是常用的 N 端连接位点，可能会提高作用的选择性，在开发新的脂肽共轭物的试验中是可行的。

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来源期刊

Bioorganic Chemistry 生物-生化与分子生物学

CiteScore

9.70

自引率

3.90%

发文量

679

审稿时长

31 days

期刊介绍： Bioorganic Chemistry publishes research that addresses biological questions at the molecular level, using organic chemistry and principles of physical organic chemistry. The scope of the journal covers a range of topics at the organic chemistry-biology interface, including: enzyme catalysis, biotransformation and enzyme inhibition; nucleic acids chemistry; medicinal chemistry; natural product chemistry, natural product synthesis and natural product biosynthesis; antimicrobial agents; lipid and peptide chemistry; biophysical chemistry; biological probes; bio-orthogonal chemistry and biomimetic chemistry. For manuscripts dealing with synthetic bioactive compounds, the Journal requires that the molecular target of the compounds described must be known, and must be demonstrated experimentally in the manuscript. For studies involving natural products, if the molecular target is unknown, some data beyond simple cell-based toxicity studies to provide insight into the mechanism of action is required. Studies supported by molecular docking are welcome, but must be supported by experimental data. The Journal does not consider manuscripts that are purely theoretical or computational in nature. The Journal publishes regular articles, short communications and reviews. Reviews are normally invited by Editors or Editorial Board members. Authors of unsolicited reviews should first contact an Editor or Editorial Board member to determine whether the proposed article is within the scope of the Journal.