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Specificity and mechanism of action of alpha-helical membrane-active peptides interacting with model and biological membranes by single-molecule force spectroscopy

机译:单分子力谱法研究α-螺旋膜活性肽与模型和生物膜相互作用的特异性和作用机理

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摘要

In this study, to systematically investigate the targeting specificity of membrane-active peptides on different types of cell membranes, we evaluated the effects of peptides on different large unilamellar vesicles mimicking prokaryotic, normal eukaryotic, and cancer cell membranes by single-molecule force spectroscopy and spectrum technology. We revealed that cationic membrane-active peptides can exclusively target negatively charged prokaryotic and cancer cell model membranes rather than normal eukaryotic cell model membranes. Using Acholeplasma laidlawii, 3T3-L1, and HeLa cells to represent prokaryotic cells, normal eukaryotic cells, and cancer cells in atomic force microscopy experiments, respectively, we further studied that the single-molecule targeting interaction between peptides and biological membranes. Antimicrobial and anticancer activities of peptides exhibited strong correlations with the interaction probability determined by single-molecule force spectroscopy, which illustrates strong correlations of peptide biological activities and peptide hydrophobicity and charge. Peptide specificity significantly depends on the lipid compositions of different cell membranes, which validates the de novo design of peptide therapeutics against bacteria and cancers.
机译:在这项研究中,为了系统地研究膜活性肽在不同类型细胞膜上的靶向特异性,我们通过单分子力谱法评估了肽对模拟原核,正常真核和癌细胞膜的不同大单层囊泡的影响。频谱技术。我们发现阳离子膜活性肽可以专门针对带负电荷的原核和癌细胞模型膜,而不是正常的真核细胞模型膜。在原子力显微镜实验中,分别使用无花果小圆虫,3T3-L1和HeLa细胞分别代表原核细胞,正常真核细胞和癌细胞,我们进一步研究了多肽和生物膜之间的单分子靶向相互作用。肽的抗微生物和抗癌活性与单分子力谱法确定的相互作用概率显示出很强的相关性,这说明了肽的生物活性与肽的疏水性和电荷之间有很强的相关性。肽的特异性很大程度上取决于不同细胞膜的脂质组成,这验证了针对细菌和癌症的肽治疗剂的从头设计。

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