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Hydrophobic modification improves the delivery of cell-penetrating peptides to eliminate intracellular pathogens in animals

细胞内 抗菌剂 抗菌肽 抗菌活性 药物输送 膜透性 细胞膜 细胞穿透肽 细胞毒性 微生物学 细胞内寄生虫 细菌 化学 细胞 生物化学 生物 体外 有机化学 遗传学
作者
Qi Tang,Peng Tan,Zhaolai Dai,Tao Wang,Shenrui Xu,Yakun Ding,Junqi Jin,Xin Zhang,Yucheng Zhang,Chenlong Zhou,Zitian Yue,Huiyang Fu,Junshu Yan,Xi Ma
出处
期刊:Acta Biomaterialia [Elsevier BV]
卷期号:157: 210-224 被引量:24
标识
DOI:10.1016/j.actbio.2022.11.055
摘要

Infections induced by intracellular pathogens are difficult to eradicate due to poor penetration of antimicrobials into cell membranes. It is of great importance to develop a new generation of antibacterial agents with dual functions of efficient cell penetration and bacterial inhibition. In this study, the association between hydrophobicity and cell-penetrating peptide delivery efficiency was investigated by fragment interception and hydrophobicity modification of natural porcine antimicrobial peptide PR-39 and the combination of cationic cell-penetrating peptide (R6) with antimicrobial peptide fragments modified with hydrophobic residues. The chimeric peptides P3I7 and P3L7, obtained through biofunctional screening, exhibited potent broad-spectrum antibacterial activity and low cytotoxicity. Moreover, P3I7 and P3L7 can effectively penetrate cells to eliminate intracellular pathogens mainly through endocytosis. The membrane destruction mechanism makes the peptides fast sterilizers and less prone to developing drug resistance. Finally, their good biocompatibility and antibacterial infection effects were verified in mice and piglets. To conclude, the chimeric peptides P3I7 and P3L7 show great potential as affordable and effective antimicrobial agents and may serve as ideal candidates for the treatment of intracellular bacterial infections. STATEMENT OF SIGNIFICANCE: The low permeability of antibacterial drugs makes infections induced by intracellular bacteria extremely difficult to treat. To address this issue, we designed chimeric peptides with dual cell-penetrating and antibacterial functions. The active peptides P3I7 and P3L7, acquired through functional screening have strong broad-spectrum antibacterial activity and powerful bactericidal effects against intracellular Staphylococcus aureus. The membrane permeation mechanism of P3I7 and P3L7 against bacteria endows fast bactericidal activity with low drug resistance. The biosafety and antibacterial activity of P3I7 and P3L7 were also validated by in vivo trials. This study provides an ideal drug candidate against intracellular bacterial infections.
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