直接观察心磷脂和抗生素对脂质 II 与 MurJ 结合的影响。

Direct observation of the influence of cardiolipin and antibiotics on lipid II binding to MurJ.

机构信息

Department of Chemistry, University of Oxford, South Parks Road, Oxford, OX1 3QZ, UK.

出版信息

Nat Chem. 2018 Mar;10(3):363-371. doi: 10.1038/nchem.2919. Epub 2018 Jan 8.

DOI:10.1038/nchem.2919

PMID:29461535

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5912511/

Abstract

Translocation of lipid II across the cytoplasmic membrane is essential in peptidoglycan biogenesis. Although most steps are understood, identifying the lipid II flippase has yielded conflicting results, and the lipid II binding properties of two candidate flippases-MurJ and FtsW-remain largely unknown. Here we apply native mass spectrometry to both proteins and characterize lipid II binding. We observed lower levels of lipid II binding to FtsW compared to MurJ, consistent with MurJ having a higher affinity. Site-directed mutagenesis of MurJ suggests that mutations at A29 and D269 attenuate lipid II binding to MurJ, whereas chemical modification of A29 eliminates binding. The antibiotic ramoplanin dissociates lipid II from MurJ, whereas vancomycin binds to form a stable complex with MurJ:lipid II. Furthermore, we reveal cardiolipins associate with MurJ but not FtsW, and exogenous cardiolipins reduce lipid II binding to MurJ. These observations provide insights into determinants of lipid II binding to MurJ and suggest roles for endogenous lipids in regulating substrate binding.

摘要

脂类 II 的跨细胞质膜易位对于肽聚糖生物合成是必不可少的。尽管大多数步骤都已被了解，但鉴定脂类 II 翻转酶的工作却产生了相互矛盾的结果，并且两种候选翻转酶（MurJ 和 FtsW）的脂类 II 结合特性在很大程度上仍然未知。在这里，我们将应用天然质谱法对这两种蛋白质进行研究，并对脂类 II 结合特性进行表征。我们观察到 FtsW 与脂类 II 的结合水平低于 MurJ，这与 MurJ 具有更高的亲和力一致。MurJ 的定点突变表明，A29 和 D269 的突变会减弱 MurJ 与脂类 II 的结合，而 A29 的化学修饰则会消除结合。抗生素雷莫拉宁可将脂类 II 从 MurJ 上解离，而万古霉素可与之结合形成稳定的 MurJ：脂类 II 复合物。此外，我们还揭示了心磷脂与 MurJ 结合而不与 FtsW 结合，并且外源性心磷脂可降低 MurJ 与脂类 II 的结合。这些观察结果为 MurJ 与脂类 II 结合的决定因素提供了深入了解，并提示内源性脂质在调节底物结合中的作用。

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本文引用的文献

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