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基于结构的建模和动力学研究表明,MurM 是一种存在于细胞质膜上的肺炎链球菌青霉素耐药决定因子。

Structure-based modeling and dynamics of MurM, a Streptococcus pneumoniae penicillin resistance determinant present at the cytoplasmic membrane.

机构信息

School of Life Science, University of Warwick, Coventry, West Midlands CV4 7AL, UK.

Centre for Fluid and Complex Systems, School of Computing, Electronics and Mathematics, University of Coventry, West Midlands CV1 5FB, UK.

出版信息

Structure. 2021 Jul 1;29(7):731-742.e6. doi: 10.1016/j.str.2021.03.001. Epub 2021 Mar 18.

Abstract

Branched Lipid II, required for the formation of indirectly crosslinked peptidoglycan, is generated by MurM, a protein essential for high-level penicillin resistance in the human pathogen Streptococcus pneumoniae. We have solved the X-ray crystal structure of Staphylococcus aureus FemX, an isofunctional homolog, and have used this as a template to generate a MurM homology model. Using this model, we perform molecular docking and molecular dynamics to examine the interaction of MurM with the phospholipid bilayer and the membrane-embedded Lipid II substrate. Our model suggests that MurM is associated with the major membrane phospholipid cardiolipin, and experimental evidence confirms that the activity of MurM is enhanced by this phospholipid and inhibited by its direct precursor phosphatidylglycerol. The spatial association of pneumococcal membrane phospholipids and their impact on MurM activity may therefore be critical to the final architecture of peptidoglycan and the expression of clinically relevant penicillin resistance in this pathogen.

摘要

分枝脂质 II 是间接交联肽聚糖形成所必需的,由 MurM 产生,MurM 是人类病原体肺炎链球菌产生高水平青霉素抗性所必需的蛋白质。我们已经解决了金黄色葡萄球菌 FemX 的 X 射线晶体结构,这是一个同工功能同源物,并以此为模板生成了 MurM 同源模型。使用该模型,我们进行分子对接和分子动力学模拟,以研究 MurM 与磷脂双层和膜嵌入的脂质 II 底物的相互作用。我们的模型表明 MurM 与主要的膜磷脂心磷脂相关联,实验证据证实 MurM 的活性受到这种磷脂的增强,并受到其直接前体磷脂酰甘油的抑制。因此,肺炎链球菌膜磷脂的空间关联及其对 MurM 活性的影响可能对肽聚糖的最终结构和该病原体中临床相关青霉素抗性的表达至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fd28/8280954/c963210d5e69/fx1.jpg

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