In Silico Molecular Docking, Synthesis and Preliminary Evaluation of Antibacterial Activity of Levofloxacin Carboxamides with Certain Amino Acids

Sarah Abdul-Razzaq makki, Shakir M. Alwan, Mayada H. Al-Qaissy
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Abstract

Levofloxacin carboxamides with certain amino acids were prepared through an amide linkage to the amino acid (glycine, histidine, or serine). These carboxamides were subjected to an in silico molecular docking evaluation on   DNA gyrase to predict their antibacterial activity using the GOLD suite. The binding affinities were very significant and encouraged the synthesis of the suggested carboxamides for intensive evaluation. These carboxamides were also subjected to Swiss ADME software to predict their ADME parameters. Levofloxacin carboxamides were prepared in high yield, and their chemical structures were confirmed by spectral analysis, such as 1H-NMR, 13C-NMR and FT-IR spectroscopy. Antibacterial activities were evaluated for the new carboxamides against two G-ve (Klebsiella and P. aeruginosa) and one G+ve (Streptococcus pneumonia) bacteria. When compared to levofloxacin, all of the synthesized carboxamides 1-3 demonstrated good activity against three types of bacteria. These carboxamides showed significant antibacterial activities against S. pneumoniae and lower activities against Klebsiella.
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含氨基酸左氧氟沙星羧胺类药物的硅分子对接、合成及抗菌活性初步评价
通过与氨基酸(甘氨酸、组氨酸或丝氨酸)的酰胺连接,制备了具有某些氨基酸的左氧氟沙星羧胺。利用GOLD套件对这些羧酰胺进行了DNA旋切酶的硅分子对接评价,以预测其抗菌活性。结合亲和性非常显著,并鼓励合成所建议的羧酰胺进行深入评价。这些carboxamide也受到瑞士ADME软件预测其ADME参数。以高收率制备了左氧氟沙星羧胺类化合物,并通过1H-NMR、13C-NMR和FT-IR等光谱分析对其化学结构进行了证实。研究了新羧酰胺对克雷伯菌和铜绿假单胞菌两种G-ve和肺炎链球菌的抑菌活性。与左氧氟沙星相比,所有合成的羧酰胺1-3对三种细菌都有良好的活性。这些羧胺对肺炎链球菌具有显著的抑菌活性,对克雷伯菌的抑菌活性较低。
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