首页> 外文期刊>Journal of enzyme inhibition and medicinal chemistry. >The RFK catalytic cycle of the pathogen Streptococcus pneumoniae shows species-specific features in prokaryotic FMN synthesis
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The RFK catalytic cycle of the pathogen Streptococcus pneumoniae shows species-specific features in prokaryotic FMN synthesis

机译:肺炎链球菌病原体的RFK催化循环在原核FMN合成中显示出物种特异性特征

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Abstract Emergence of multidrug-resistant bacteria forces us to explore new therapeutic strategies, and proteins involved in key metabolic pathways are promising anti-bacterial targets. Bifunctional flavin-adenine dinucleotide (FAD) synthetases (FADS) are prokaryotic enzymes that synthesise the flavin mononucleotide (FMN) and FAD cofactors. The FADS from the human pathogen?Streptococcus pneumoniae (SpnFADS)–causative agent of pneumonia in humans???shows relevant catalytic dissimilarities compared to other FADSs. Here, by integrating thermodynamic and kinetic data, we present a global description of the riboflavin kinase activity of SpnFADS, as well as of the inhibition mechanisms regulating this activity. Our data shed light on biophysical determinants that modulate species-specific conformational changes leading to catalytically competent conformations, as well as binding rates and affinities of substrates versus products. This knowledge paves the way for the development of tools???that taking advantage of the regulatory dissimilarities during FMN biosynthesis in different species???might be used in the discovery of specific anti-pneumococcal drugs.
机译:摘要多药耐药细菌的出现迫使我们探索新的治疗策略,而关键代谢途径中涉及的蛋白质是有希望的抗菌靶标。双功能黄素腺嘌呤二核苷酸(FAD)合成酶(FADS)是合成黄素单核苷酸(FMN)和FAD辅因子的原核酶。来自人类病原体的肺炎链球菌-肺炎链球菌(SpnFADS)是人类肺炎的致病因子-与其他FADS相比,显示出相关的催化差异。在这里,通过综合热力学和动力学数据,我们对SpnFADS的核黄素激酶活性以及调节这种活性的抑制机制进行了全面描述。我们的数据揭示了生物物理决定簇,这些决定簇调节物种特异性的构象变化,从而导致具有催化能力的构象,以及底物与产品的结合率和亲和力。这一知识为工具的开发铺平了道路。在不同种类的FMN生物合成过程中利用调节差异的优势可能被用于发现特定的抗肺炎球菌药物。

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