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A synergistic role for two predicted inner membrane proteins of Escherichia coli in cell envelope integrity

机译:两种预测内膜蛋白在细胞包络完整性中的两个预测内膜蛋白的协同作用

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The bacterial cytoplasmic membrane is a principal site of protein translocation, lipid and peptidoglycan biogenesis, signal transduction, transporters and energy generating components of the respiratory chain. Although 25-30% of bacterial proteomes consist of membrane proteins, a comprehensive understanding of their influence on fundamental cellular processes is incomplete. Here, we show that YciB and DcrB, two small cytoplasmic membrane proteins of previously unknown functions, play an essential synergistic role in maintaining cell envelope integrity of Escherichia coli. Lack of both YciB and DcrB results in pleiotropic cell defects including increased levels of lipopolysaccharide, membrane vesiculation, dynamic shrinking and extension of the cytoplasmic membrane accompanied by lysis and cell death. The stalling of an abundant outer membrane lipoprotein, Lpp, at the periplasmic face of the inner membrane leads to lethal inner membrane-peptidoglycan linkages. Additionally, the periplasmic chaperone Skp contributes to yciB dcrB mutant cell death by possibly mistargeting stalled porins into the inner membrane. Consistent with the idea of a compromised envelope in the yciB dcrB mutant, multiple envelope stress response systems are induced, with Cpx signal transduction being required for growth. Taken together, our results suggest a fundamental role for YciB and DcrB in cell envelope biogenesis.
机译:细菌细胞质膜是蛋白质易位,脂质和肽聚糖生物发生,信号转导,转运蛋白和能量产生呼吸链的主要部位。虽然25-30%的细菌蛋白质蛋白由膜蛋白组成,但综合了解它们对基本细胞过程的影响是不完整的。在这里,我们表明Ycib和DCRB,两种小型细胞质膜蛋白的先前未知的功能,在维持大肠杆菌的细胞包络完整性中起重要的协同作用。缺乏YCIB和DCRB导致脂肪细胞缺陷,包括伴有裂解和细胞死亡的细胞质膜的增加水平,膜混凝剂,动态收缩和延伸的细胞质膜。在内膜的周质面上的富有外膜脂蛋白,LPP的放路导致致死的内膜 - 肽聚糖键。另外,周质伴侣SKP通过可能将被停滞的孔腔捕获到内膜中有助于Ycib DCRB突变细胞死亡。与YCIB DCRB突变体中受损信封的思想一致,诱导多个包络应力响应系统,CPX信号转换是增长所必需的。我们的结果表明,ycib和DCRB在细胞包膜生物发生中的基本作用。

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