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Lipids assist the membrane insertion of a BAM-independent outer membrane protein

机译:脂质帮助膜独立于BAM的外膜蛋白的插入

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摘要

Like several other large, multimeric bacterial outer membrane proteins (OMPs), the assembly of the Klebsiella oxytoca OMP PulD does not rely on the universally conserved β-barrel assembly machinery (BAM) that catalyses outer membrane insertion. The only other factor known to interact with PulD prior to or during outer membrane targeting and assembly is the cognate chaperone PulS. Here, in vitro translation-transcription coupled PulD folding demonstrated that PulS does not act during the membrane insertion of PulD, and engineered in vivo site-specific cross-linking between PulD and PulS showed that PulS binding does not prevent membrane insertion. In vitro folding kinetics revealed that PulD is atypical compared to BAM-dependent OMPs by inserting more rapidly into membranes containing E. coli phospholipids than into membranes containing lecithin. PulD folding was fast in diC14:0-phosphatidylethanolamine liposomes but not diC14:0-phosphatidylglycerol liposomes, and in diC18:1-phosphatidylcholine liposomes but not in diC14:1-phosphatidylcholine liposomes. These results suggest that PulD efficiently exploits the membrane composition to complete final steps in insertion and explain how PulD can assemble independently of any protein-assembly machinery. Lipid-assisted assembly in this manner might apply to other large OMPs whose assembly is BAM-independent.
机译:像其他几个大型的多聚细菌外膜蛋白(OMP)一样,产酸克雷伯菌OMP PulD的组装不依赖于催化外膜插入的普遍保守的β-桶组装机械(BAM)。已知在外膜靶向和组装之前或期间与PulD相互作用的唯一其他因素是同源伴侣PulS。在这里,体外翻译-转录偶联的PulD折叠表明PulS在PulD的膜插入过程中不起作用,PulD和PulS之间进行的体内体内位点特异性交联表明PulS结合不会阻止膜的插入。体外折叠动力学表明,与BAM依赖的OMP相比,PulD具有非典型的特征,它比含卵磷脂的膜更快速地插入含大肠杆菌磷脂的膜中。在diC14:0-磷脂酰乙醇胺脂质体中,PulD折叠较快,而在diC14:0-磷脂酰甘油脂质体中,PulD折叠较快;而在diC18:1-磷脂酰胆碱脂质体中,PulD折叠较快,但在diC14:1-磷脂酰胆碱脂质体中却没有。这些结果表明,PulD有效地利用了膜成分来完成插入的最终步骤,并解释了PulD如何能够独立于任何蛋白质组装机器进行组装。以这种方式进行脂质辅助的组装可能适用于其组装与BAM无关的其他大型OMP。

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