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Characterization of Natural Products as Inhibitors of Shikimate Dehydrogenase from Methicillin-Resistant Staphylococcus aureus: Kinetic and Molecular Dynamics Simulations, and Biological Activity Studies

咖啡酸 莽草酸途径 生物化学 金黄色葡萄球菌 化学 磷酸戊糖途径 氨基酸 芦丁 芳香族氨基酸 微生物学 生物 细菌 糖酵解 抗氧化剂 遗传学
作者
Noé Fabián Corral-Rodríguez,Valeria Itzel Moreno-Contreras,Erick Sierra‐Campos,Mónica Valdez‐Solana,Jorge Cisneros-Martínez,Alfredo Téllez‐Valencia,Claudia Avitia‐Domínguez
出处
期刊:Biomolecules [MDPI AG]
卷期号:15 (8): 1137-1137
标识
DOI:10.3390/biom15081137
摘要

Antibiotic resistance is considered to be one of the most complex health obstacles of our time. Methicillin-resistant Staphylococcus aureus (MRSA) represents a global health challenge due to its broad treatment resistance capacity, resulting in high mortality rates. The shikimate pathway (SP) is responsible for the biosynthesis of chorismate from glycolysis and pentose phosphate pathway intermediates. This pathway plays a crucial role in producing aromatic amino acids, folates, ubiquinone, and other secondary metabolites in bacteria. Notably, SP is absent in humans, which makes it a specific and potential therapeutic target to explore for discovering new antibiotics against MRSA. The present study characterized in vitro and in silico natural products as inhibitors of the shikimate dehydrogenase from methicillin-resistant S. aureus (SaSDH). The results showed that, from the set of compounds studied, phloridzin, rutin, and caffeic acid were the most potent inhibitors of SaSDH, with IC50 values of 140, 160, and 240 µM, respectively. Furthermore, phloridzin showed a mixed-type inhibition mechanism, whilst rutin and caffeic acid showed non-competitive mechanisms. The structural characterization of the SaSDH–inhibitor complex indicated that these compounds interacted with amino acids from the catalytic site and formed stable complexes. In biological activity studies against MRSA, caffeic acid showed an MIC of 2.2 mg/mL. Taken together, these data encourage using these compounds as a starting point for developing new antibiotics based on natural products against MRSA.

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