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首页> 外文期刊>Clinical and diagnostic laboratory immunology >Augmentation of the Lipopolysaccharide-Neutralizing Activities of Human Cathelicidin CAP18/LL-37-Derived Antimicrobial Peptides by Replacement with Hydrophobic and Cationic Amino Acid Residues
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Augmentation of the Lipopolysaccharide-Neutralizing Activities of Human Cathelicidin CAP18/LL-37-Derived Antimicrobial Peptides by Replacement with Hydrophobic and Cationic Amino Acid Residues

机译:通过疏水和阳离子氨基酸残基的替代增强人​​Cathelicidin CAP18 / LL-37衍生的抗菌肽的脂多糖中和活性。

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摘要

Mammalian myeloid and epithelial cells express various peptide antibiotics (such as defensins and cathelicidins) that contribute to the innate host defense against invading microorganisms. Among these peptides, human cathelicidin CAP18/LL-37 (L1 to S37) possesses not only potent antibacterial activity against gram-positive and gram-negative bacteria but also the ability to bind to gram-negative lipopolysaccharide (LPS) and neutralize its biological activities. In this study, to develop peptide derivatives with improved LPS-neutralizing activities, we utilized an 18-mer peptide (K15 to V32) of LL-37 as a template and evaluated the activities of modified peptides by using the CD14+ murine macrophage cell line RAW 264.7 and the murine endotoxin shock model. By replacement of E16 and K25 with two L residues, the hydrophobicity of the peptide (18-mer LL) was increased, and by further replacement of Q22, D26, and N30 with three K residues, the cationicity of the peptide (18-mer LLKKK) was enhanced. Among peptide derivatives, 18-mer LLKKK displayed the most powerful LPS-neutralizing activity: it was most potent at binding to LPS, inhibiting the interaction between LPS and LPS-binding protein, and attaching to the CD14 molecule, thereby suppressing the binding of LPS to CD14+ cells and attenuating production of tumor necrosis factor alpha (TNF-α) by these cells. Furthermore, in the murine endotoxin shock model, 18-mer LLKKK most effectively suppressed LPS-induced TNF-α production and protected mice from lethal endotoxin shock. Together, these observations indicate that the LPS-neutralizing activities of the amphipathic human CAP18/LL-37-derived 18-mer peptide can be augmented by modifying its hydrophobicity and cationicity, and that 18-mer LLKKK is the most potent of the peptide derivatives, with therapeutic potential for gram-negative bacterial endotoxin shock.
机译:哺乳动物的髓样和上皮细胞表达多种肽类抗生素(例如防御素和cathelicidins),这些肽类有助于先天宿主对入侵微生物的防御。在这些肽中,人cathelicidin CAP18 / LL-37(L 1 至S 37 )不仅具有针对革兰氏阳性和革兰氏阴性细菌的有效抗菌活性,而且还具有与革兰氏阴性脂多糖(LPS)结合并中和其生物学活性的能力。在这项研究中,为了开发具有改善的LPS中和活性的肽衍生物,我们以LL-37的18-mer肽(K 15 至V 32 )为模板并使用CD14 + 鼠巨噬细胞RAW 264.7细胞株和鼠内毒素休克模型评估了修饰肽的活性。通过用两个L残基替换E 16 和K 25 ,可增加肽(18-mer LL)的疏水性,并进一步替换Q 22 ,D 26 和N 30 带有三个K残基,增强了该肽(18-mer LLKKK)的阳离子性。在肽衍生物中,18-mer LLKKK显示出最强大的LPS中和活性:最有效地结合LPS,抑制LPS和LPS结合蛋白之间的相互作用,并附着于CD14分子,从而抑制LPS的结合抑制CD14 + 细胞的生长,并减弱这些细胞产生的肿瘤坏死因子α(TNF-α)。此外,在鼠类内毒素休克模型中,18-mer LLKKK最有效地抑制LPS诱导的TNF-α产生,并保护小鼠免受致命的内毒素休克。总之,这些观察结果表明,两亲性人CAP18 / LL-37衍生的18-mer肽的LPS中和活性可以通过改变其疏水性和阳离子性来增强,并且18-mer LLKKK是最有效的肽衍生物具有革兰氏阴性细菌内毒素休克的治疗潜力。

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