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牛髓源抗菌肽-18(BMAP-18)及其类似物的细胞选择性、作用机制和脂多糖中和活性。

Cell selectivity, mechanism of action and LPS-neutralizing activity of bovine myeloid antimicrobial peptide-18 (BMAP-18) and its analogs.

机构信息

Department of Bio-Materials, Graduate School and Research Center for Proteineous Materials, Chosun University, Gwangju 501-759, Republic of Korea.

出版信息

Peptides. 2011 Jun;32(6):1123-30. doi: 10.1016/j.peptides.2011.03.024. Epub 2011 Apr 8.

Abstract

To develop novel antimicrobial peptides (AMPs) with improved cell selectivity and potent LPS-neutralizing activity, we synthesized an 18 N-terminal residues peptide (BAMP-18) of bovine myeloid antimicrobial peptide-27 (BMAP-27) and its analogs (BMAP-18-W, BMAP-18-L, BMAP-18-I and BMAP-18-f). BMAP-18 and its analogs displayed much higher cell selectivity (about 4-97-fold increased) as compared to parental BMAP-27 because of their decreased hemolytic activity and retained antimicrobial activity. BMAP-27 caused near-complete dye leakage from bacterial-membrane-mimicking vesicles even at very low concentration of 0.5μM, whereas BMAP-18 and its analogs induced very little dye leakage (less than 40%) even at 16μM. These peptides induced near-complete membrane depolarization of Staphylococcus aureus cells under their MIC (4μM). These results suggests that BMAP-18 and its analogs exhibit lethality toward microbes due to their ability to form small channels that permit the transit of ions or protons, but not molecules as large as calcein, and not by the membrane-disruption/perturbation mode. BMAP-18 and its analogs significantly inhibited nitric oxide (NO) production or tumor necrosis factor-α (TNF-α) release in LPS-stimulated mouse macrophage RAW264.7 cells at 10μM. In particular, BMAP-18-W showed LPS-neutralizing activity comparable to that of BMAP-27. There was a significant linear correlation between the increase in the hydrophobicity of peptides and LPS-neutralizing activity. Although BMAP-18-W has lower hydrophobicity than BMAP-18-L, it showed higher LPS-neutralizing activity as compared to BMAP-18-L. This result suggests other important parameters of AMPs may be involved in their LPS-neutralizing activity, as well as positive charge and hydrophobicity.

摘要

为了开发具有改善的细胞选择性和有效中和 LPS 活性的新型抗菌肽 (AMPs),我们合成了牛髓源抗菌肽-27 (BMAP-27) 的 18 个 N 端残基肽 (BAMP-18) 及其类似物 (BMAP-18-W、BMAP-18-L、BMAP-18-I 和 BMAP-18-f)。与亲本 BMAP-27 相比,BAMP-18 及其类似物的细胞选择性高得多(约增加 4-97 倍),因为它们的溶血活性降低而保留了抗菌活性。BMAP-27 甚至在非常低的浓度 0.5μM 下也能引起类似细菌膜的囊泡中染料的几乎完全泄漏,而 BMAP-18 和其类似物即使在 16μM 时也只能引起很少的染料泄漏(小于 40%)。这些肽在其 MIC(4μM)下使金黄色葡萄球菌细胞的膜几乎完全去极化。这些结果表明,BAMP-18 和其类似物由于能够形成允许离子或质子通过的小通道,而不是像 calcein 那样大的分子,因此对微生物具有致死性,而不是通过膜破坏/干扰模式。BAMP-18 和其类似物在 10μM 时显著抑制 LPS 刺激的小鼠巨噬细胞 RAW264.7 细胞中一氧化氮 (NO) 的产生或肿瘤坏死因子-α (TNF-α) 的释放。特别是,BMAP-18-W 表现出与 BMAP-27 相当的 LPS 中和活性。肽的疏水性增加与 LPS 中和活性之间存在显著的线性相关性。尽管 BMAP-18-W 的疏水性低于 BMAP-18-L,但与 BMAP-18-L 相比,它表现出更高的 LPS 中和活性。这一结果表明,AMP 的其他重要参数可能参与其 LPS 中和活性,以及正电荷和疏水性。

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