Development of Novel Indole and Coumarin Derivatives as Antibacterial Agents That Target Histidine Kinase in S. aureus

Lisha K. Poonacha, Rashmi Ramesh, Akshay Ravish, Arunkumar Mohan, Pradeep M. Uppar, Prashant K. Metri, Nanjunda Swamy Shivananju, Santosh L. Gaonkar, Shubha Gopal, Alexey Yu Sukhorukov, Vijay Pandey, Priya Babu Shubha, Basappa Basappa
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Abstract

Heterocyclic compounds can specifically regulate bacterial development by targeting specific bacterial enzymes and metabolic pathways. The ESKAPE pathogens are multidrug-resistant and cause nosocomial infections, which is one of the greatest challenges in clinical practice. The search for novel agents to combat resistant bacteria has become one of the most important areas of antibacterial research today. Heterocyclic compounds offer a valuable strategy in the fight against resistance as they can be designed to interact with bacterial targets that are less prone to developing resistance mechanisms. Bacterial histidine kinases (HKs), which are a component of two-component bacterial systems, are a promising target for new antibacterial compounds. We have designed and synthesized novel indole derivatives as antibacterial agents. Among the series, indole-coumarin (4b) and bisindole (4e) have shown the best inhibitory activity against S. aureus. Further, in silico docking studies show that compounds 4b and 4e could target histidine kinases in bacteria.
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针对金黄色葡萄球菌组氨酸激酶的新型吲哚和香豆素衍生物的研究进展
杂环化合物可以通过靶向特定的细菌酶和代谢途径特异性调节细菌的发育。ESKAPE病原菌具有多重耐药性,可引起医院感染,是临床实践中面临的最大挑战之一。寻找对抗耐药细菌的新型药物已成为当今抗菌研究的最重要领域之一。杂环化合物为抵抗耐药性提供了一种有价值的策略,因为它们可以被设计成与不太容易产生耐药性机制的细菌靶点相互作用。细菌组氨酸激酶(HKs)是双组分细菌系统的一个组成部分,是新型抗菌化合物的一个有希望的靶点。我们设计并合成了新型吲哚类抗菌剂。其中,吲哚-香豆素(4b)和双吲哚(4e)对金黄色葡萄球菌的抑制活性最好。此外,硅对接研究表明,化合物4b和4e可以靶向细菌中的组氨酸激酶。
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