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Design and Synthesis of Aryl Ether Inhibitors of the Bacillus Anthracis Enoyl-ACP Reductase

机译:炭疽芽孢杆菌烯酰基-ACP还原酶的芳醚抑制剂的设计与合成

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The problem of increasing bacterial resistance to the current generation of antibiotics is well documented. Known resistant pathogens such as methicillin-resistant Staphylococcus aureus are becoming more prevalent, while the potential exists for developing drug-resistant pathogens for use as bioweapons, such as Bacillus anthracis. The biphenyl ether antibacterial agent, triclosan, exhibits broad-spectrum activity by targeting the fatty acid biosynthet-ic pathway through inhibition of enoyl-acyl carrier protein reductase (ENR) and provides a potential scaffold for the development of new, broad-spectrum antibiotics. We used a structure-based approach to develop novel aryl ether analogues of triclosan that target ENR, the product of the fabl gene, from B. anthracis (BaENR). Structure-based design methods were used for the expansion of the compound series including X-ray crystal structure determination, molecular docking, and QSAR methods. Structural modifications were made to both phenyl rings of the 2-phenoxy-phenyl core. A number of compounds exhibited improved potency against BaENR and increased efficacy against both the Sterne strain of B. anthracis and the methicillin-resistant strain of S. aureus. X-ray crystal structures of BaENR in complex with triclosan and two other compounds help explain the improved efficacy of the new compounds and suggest future rounds of optimization that might be used to improve their potency.
机译:已有文献证明增加细菌对当前一代抗生素的抗性的问题。已知的耐药病原体(例如耐甲氧西林的金黄色葡萄球菌)正变得越来越普遍,而存在开发用作生物武器的耐药病原体(例如炭疽芽孢杆菌)的潜力。联苯醚抗菌剂三氯生通过抑制烯酰酰基载体蛋白还原酶(ENR)靶向脂肪酸生物合成途径,具有广谱活性,并为开发新型广谱抗生素提供了潜在的支架。我们使用基于结构的方法开发了新的三氯生芳基醚类似物,该类似物靶向炭疽芽胞杆菌(BaENR)的fabl基因产物ENR。基于结构的设计方法用于扩展化合物系列,包括X射线晶体结构确定,分子对接和QSAR方法。对2-苯氧基-苯基核的两个苯环进行了结构修饰。许多化合物显示出对BaENR的增强的效力,并且对炭疽芽孢杆菌的Sterne菌株和金黄色葡萄球菌的耐甲氧西林的菌株均具有增强的功效。 BaENR与三氯生和其他两种化合物配合使用的X射线晶体结构有助于说明新化合物的功效提高,并建议未来进行一轮优化,以提高其功效。

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