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首页> 外文期刊>Journal of Medicinal Chemistry >A new DNA gyrase inhibitor subclass of the cyclothialidine family based on a bicyclic dilactam-lactone scaffold. Synthesis and antibacterial properties
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A new DNA gyrase inhibitor subclass of the cyclothialidine family based on a bicyclic dilactam-lactone scaffold. Synthesis and antibacterial properties

机译:一种基于双环双内酰胺-内酯支架的环噻啶家族的新的DNA促旋酶抑制剂亚类。合成与抗菌性能

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摘要

The DNA gyrase inhibitor cyclothialidine had been shown to be a valuable lead structure for the discovery of new antibacterial classes able to overcome bacterial resistance to clinically used drugs. Bicyclic lactone derivatives containing in their 12-14-membered ring a thioamide functionality were reported previously to exhibit potent antibacterial activity against Gram-positive bacteria. Moderate in vivo efficacy, however, was demonstrated only for derivatives bearing hydrophilic substituents, which were found to have a favorable impact on pharmcokinetics, and to reduce metabolic degradation, in particular glucuronidation. The incorporation of an additional amide unit into the 14-membered monolactam-lactone scaffold of cyclothialidine analogues provided a new "dilactam" subclass of DNA gyrase inhibitors of inherently higher polarity. After adjusting their lipophilicity by methyl-halogen exchange at the benzene ring, compounds of this series did not require the thioamide functionality to exert a decent antibacterial potency and consequently exhibited improved pharmacokinetic properties resulting in a pronounced in vivo efficacy in a mouse septicaemia infection model.
机译:对于发现能够克服细菌对临床使用药物的耐药性的新型抗菌剂而言,DNA回旋酶抑制剂环噻啶已被证明是有价值的先导结构。先前已经报道了在其12-14元环中含有硫酰胺官能团的双环内酯衍生物表现出对革兰氏阳性细菌的有效抗菌活性。然而,仅对带有亲水性取代基的衍生物证明了中等的体内功效,发现该衍生物对药物动力学具有有利的影响,并减少了代谢降解,特别是葡萄糖醛酸化。将额外的酰胺单元掺入环噻啶类似物的14元单内酰胺-内酯支架中,提供了固有地具有更高极性的DNA回旋酶抑制剂的新的“双内酰胺”亚类。在通过苯环上的甲基卤素交换调节亲脂性之后,该系列化合物不需要硫酰胺官能团发挥适度的抗菌效力,因此在小鼠败血病感染模型中表现出明显的体内药效,从而具有明显的体内功效。

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