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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >How kanamycin A interacts with bacterial and mammalian mimetic membranes
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How kanamycin A interacts with bacterial and mammalian mimetic membranes

机译:卡那霉素如何与细菌和哺乳动物模拟膜相互作用

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摘要

Biological membranes are natural barriers to the transport of molecules and drugs within human bodies. Many antibacterial agents need to cross these membranes to reach their target and elicit specific effects. Kanamycin A belongs to the family of aminoglycoside antibiotics that target cellular RNA to inhibit bacterial and viral replication. Previous studies have shown that aminoglycosides bind to mammalian but disrupt bacterial membranes. In this study, molecular dynamics (MD) simulations and infrared (IR) spectroscopy were applied to investigate the initial, first key interactions of kanamycin A, as a representative aminoglycoside, with both bacterial and mammalian lipid bilayers at the molecular level. Computational studies revealed strong hydrogen bonding interactions between the hydroxyl and amino groups of the aminoglycoside with the ester carbonyl and phosphate groups of the lipids. IR spectroscopy provided experimental verification of the important role of the lipid's ester carbonyl, phosphate and hydroxyl groups for aminoglycoside binding. The bacterial membrane became disordered upon aminoglycoside addition, whereas the mammalian membrane became stiffer and more ordered. This indicates the bacterial membrane disruption observed by previous studies.
机译:生物膜是人体中分子和药物运输的天然障碍。许多抗菌剂需要穿过这些膜以达到其目标和引发特定效果。卡那霉素A属于靶向细胞RNA以抑制细菌和病毒复制的氨基糖苷类抗生素系列。以前的研究表明,氨基糖苷与哺乳动物结合但破坏了细菌膜。在该研究中,应用分子动力学(MD)模拟和红外(IR)光谱法研究Kanamycin A,作为代表性氨基糖苷的初始,第一关键相互作用,其中细菌和哺乳动物脂质双层在分子水平。计算研究揭示了氨基糖苷类的羟基和氨基与脂质的酯羰基和磷酸盐基团之间的强氢键相互作用。 IR光谱提供了脂质的酯羰基,磷酸盐和羟基用于氨基糖苷结合的重要作用的实验验证。细菌膜在加成氨基糖苷时变得混乱,而哺乳动物膜变得更易于越来越多。这表明先前研究观察的细菌膜破坏。

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