发现针对耐多药粪肠球菌细胞壁生物合成的潜在天然疗法:一种计算视角。

IF 5.7 2区 生物学 Q1 BIOLOGY Biology Direct Pub Date : 2024-11-05 DOI:10.1186/s13062-024-00538-2
Km Rakhi, Monika Jain, Amit Kumar Singh, Mohd Sajid Ali, Hamad A Al-Lohedan, Jayaraman Muthukumaran
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引用次数: 0

摘要

背景:确定参与肽聚糖生物合成途径的关键酶的治疗抑制剂对于开发针对耐多药粪肠球菌 V583 的新疗法至关重要。MurM 是这一途径中的一个重要酶,在该细菌的细胞壁合成过程中发挥着重要作用,因此成为新型抗菌策略的一个有吸引力的药物靶点。本研究探索了天然化合物作为 MurM 抑制剂的潜力,旨在发现有潜力的候选药物,为未来的治疗开发奠定基础:方法:对 MurM 的三维结构进行了预测和优化,并通过与相关结构的比较分析了其结合口袋。对 COCONUT 数据库中的 470,000 多种天然化合物进行了虚拟高通量筛选(vHTS)。根据它们的利宾斯基特征、ADME特征、毒性特征、估计的结合自由能(ΔG)和估计的抑制常数(Ki),筛选出了最重要的候选先导化合物。相互作用模式分析用于评估抑制剂与 MurM 结合袋中关键残基之间的非共价相互作用。进行了 300 ns 的分子动力学模拟,以评估这些抑制剂的结构稳定性及其对 MurM 酶的影响:结果:确定了三个先导化合物-CNP0056520、CNP0126952 和 CNP0248480,并将其列为优先化合物,其估计 ΔG 范围为 - 9.35 至 - 7.9 kcal/mol。分子动力学模拟显示,候选抑制剂对 MurM 的整体结构和动力学影响极小,能形成稳定的蛋白质配体复合物。候选抑制剂与 MurM 结合口袋中的关键残基之间的几种非共价相互作用支持了这些相互作用:这些研究结果表明,已确定的候选天然产物可作为 MurM 的有效抑制剂,从而有可能开发出针对耐多药粪肠球菌细胞壁生物合成的新型疗法。
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Discovery of potential natural therapeutics targeting cell wall biosynthesis in multidrug-resistant Enterococcus faecalis: a computational perspective.

Background: Identifying therapeutic inhibitors of crucial enzymes involved in the peptidoglycan biosynthesis pathway is pivotal for developing new treatments against multidrug-resistant Enterococcus faecalis V583. MurM, an essential enzyme in this pathway, plays a significant role in the bacterium's cell wall synthesis, making it an attractive druggable target for novel antimicrobial strategies. This study explored the potential of natural compounds as inhibitors of MurM, aiming to discover promising drug candidates that could serve as the foundation for future therapeutic development.

Methods: The three-dimensional structure of MurM was predicted, optimized, and its binding pocket was analyzed by comparing it with related structures. Over 4,70,000 natural compounds from the COCONUT database were subjected to virtual high-throughput screening (vHTS). The top lead candidates were selected based on their Lipinski's profile, ADME profile, toxicity profile, estimated binding free energy (ΔG) and estimated inhibition constant (Ki). Interaction pattern analysis was used to evaluate the non-covalent interactions between the inhibitors and key residues in MurM's binding pocket. Molecular dynamics simulations were performed over 300 ns to assess the structural stability and impact of these inhibitors on MurM's enzyme.

Results: Three lead compounds-CNP0056520, CNP0126952, and CNP0248480-were identified and prioritized with estimated ΔG ranging from - 9.35 to -7.9 kcal/mol. Molecular dynamics simulations revealed minimal impact on MurM's overall structure and dynamics, with the candidate inhibitors forming stable protein-ligand complexes. These interactions were supported by several non-covalent interactions between the candidate inhibitors and key residues within MurM's binding pocket.

Conclusion: These findings suggest that the identified natural product candidates could serve as promising inhibitors of MurM, potentially leading to novel therapeutics targeting cell wall biosynthesis in multidrug-resistant E. faecalis.

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来源期刊
Biology Direct
Biology Direct 生物-生物学
CiteScore
6.40
自引率
10.90%
发文量
32
审稿时长
7 months
期刊介绍: Biology Direct serves the life science research community as an open access, peer-reviewed online journal, providing authors and readers with an alternative to the traditional model of peer review. Biology Direct considers original research articles, hypotheses, comments, discovery notes and reviews in subject areas currently identified as those most conducive to the open review approach, primarily those with a significant non-experimental component.
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