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Unveiling the Importance of Amide Protons in CSP:ComD Interactions in Streptococcus pneumoniae

机译:揭示酰胺质子在CSP中的重要性:链球菌肺炎料的COMD相互作用

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Streptococcus pneumoniae is an opportunistic pathogen that can cause diseases ranging from mild respiratory infections to life-threatening conditions such as pneumonia, meningitis, and bacteremia. S. pneumoniae pathogenicity is dependent on the action of a 17-amino acid peptide pheromone, termed competence stimulating peptide (CSP) that controls the competence regulon, a quorum sensing (QS) circuit. Therefore, intercepting QS could have therapeutic implications in treating pneumococcal infections while avoiding emerging antimicrobial resistance. In this study, we set out to evaluate the impact of amide protons on CSP activity and metabolic stability through systematic N-methylation. Our results indicate that the majority of amide protons are critical for CSP activity, either through direct interactions with the cognate receptor or by stabilizing the bioactive conformation. Importantly, we identified several N-methyl CSP analogs, namely, CSP1(15)-N-Me-K6 and CSP1(15)-N-Me-F7, that retain their biological activity while exhibiting enhanced metabolic stability. These analogs are privileged scaffolds for the design of CSP-based QS modulators with drug-like properties.
机译:肺炎链球菌是一种机会主义病原体,可以导致疾病从轻度呼吸道感染到肺炎,脑膜炎和菌血症等危及生命的病症。 S.肺炎致病性依赖于17-氨基酸肽信息素的作用,称为控制能力调节件的竞争力刺激肽(CSP),批量传感(QS)电路。因此,拦截QS可以具有治疗肺炎球菌感染的治疗意义,同时避免出现的抗微生物抗性。在本研究中,我们首先通过系统的N-甲基化评估酰胺质子对CSP活性和代谢稳定性的影响。我们的结果表明,大多数酰胺质子对于CSP活性至关重要,通过与同源受体的直接相互作用或通过稳定生物活性构象来稳定。重要的是,我们鉴定了几种N-甲基CSP类似物,即CSP1(15)-N-ME-K6和CSP1(15)-N-ME-F7,其在表现出增强的代谢稳定性的同时保持其生物活性。这些类似物是特权脚手架,用于设计基于CSP的QS调制器,具有类似药物的性质。

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