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Small membranous proteins of the TorE/NapE family, crutches for cognate respiratory systems in Proteobacteria

机译:TorE / NapE家族的小膜蛋白,用于变形杆菌中同源呼吸系统的拐杖

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In this report, we investigate small proteins involved in bacterial alternative respiratory systems that improve the enzymatic efficiency through better anchorage and multimerization of membrane components. Using the small protein TorE of the respiratory TMAO reductase system as a model, we discovered that TorE is part of a subfamily of small proteins that are present in proteobacteria in which they play a similar role for bacterial respiratory systems. We reveal by microscopy that, in Shewanella oneidensis MR1, alternative respiratory systems are evenly distributed in the membrane contrary to what has been described for Escherichia coli . Thus, the better efficiency of the respiratory systems observed in the presence of the small proteins is not due to a specific localization in the membrane, but rather to the formation of membranous complexes formed by TorE homologs with their c -type cytochrome partner protein. By an in vivo approach combining Clear Native electrophoresis and fluorescent translational fusions, we determined the 4:4 stoichiometry of the complexes. In addition, mild solubilization of the cytochrome indicates that the presence of the small protein reinforces its anchoring to the membrane. Therefore, assembly of the complex induced by this small protein improves the efficiency of the respiratory system.
机译:在此报告中,我们研究了参与细菌替代呼吸系统的小蛋白,这些蛋白通过更好的固定和膜成分的多聚化提高了酶的效率。使用呼吸TMAO还原酶系统的小蛋白TorE作为模型,我们发现TorE是蛋白菌中存在的小蛋白亚家族的一部分,其中它们在细菌呼吸系统中起着相似的作用。我们通过显微镜揭示,在Shewanella oneidensis MR1​​中,与对大肠杆菌的描述相反,替代呼吸系统均匀地分布在膜中。因此,在小蛋白存在下观察到的呼吸系统的更好效率不是由于膜中的特定定位,而是由于TorE同系物与其c型细胞色素伴侣蛋白形成的膜复合物的形成。通过结合Clear Native电泳和荧光翻译融合的体内方法,我们确定了复合物的4:4化学计量。另外,细胞色素的温和溶解表明小蛋白的存在增强了其锚定在膜上的能力。因此,由这种小蛋白质诱导的复合物的组装提高了呼吸系统的效率。

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