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荚膜红细菌中,cbb3型细胞色素c氧化酶的完全活性和铜稳态需要两种周质铜伴侣之间的合作。

Cooperation between two periplasmic copper chaperones is required for full activity of the cbb3 -type cytochrome c oxidase and copper homeostasis in Rhodobacter capsulatus.

作者信息

Trasnea Petru-Iulian, Utz Marcel, Khalfaoui-Hassani Bahia, Lagies Simon, Daldal Fevzi, Koch Hans-Georg

机构信息

Institut für Biochemie und Molekularbiologie, ZBMZ, Stefan-Meier-Strasse 17, 79104, Freiburg, Germany.

Fakultät für Biologie, Albert-Ludwigs-Universität Freiburg, 79104, Freiburg, Germany.

出版信息

Mol Microbiol. 2016 Apr;100(2):345-61. doi: 10.1111/mmi.13321. Epub 2016 Feb 28.

Abstract

Copper (Cu) is an essential micronutrient that functions as a cofactor in several important enzymes, such as respiratory heme-copper oxygen reductases. Yet, Cu is also toxic and therefore cells engage a highly coordinated Cu uptake and delivery system to prevent the accumulation of toxic Cu concentrations. In this study, we analyzed Cu delivery to the cbb3 -type cytochrome c oxidase (cbb3 -Cox) of Rhodobacter capsulatus. We identified the PCuA C-like periplasmic chaperone PccA and analyzed its contribution to cbb3 -Cox assembly. Our data demonstrate that PccA is a Cu-binding protein with a preference for Cu(I), which is required for efficient cbb3 -Cox assembly, in particular, at low Cu concentrations. By using in vivo and in vitro cross-linking, we show that PccA forms a complex with the Sco1-homologue SenC. This complex is stabilized in the absence of the cbb3 -Cox-specific assembly factors CcoGHIS. In cells lacking SenC, the cytoplasmic Cu content is significantly increased, but the simultaneous absence of PccA prevents this Cu accumulation. These data demonstrate that the interplay between PccA and SenC not only is required for Cu delivery during cbb3 -Cox assembly but also regulates Cu homeostasis in R. capsulatus.

摘要

铜(Cu)是一种必需的微量营养素,在几种重要的酶中作为辅因子发挥作用,如呼吸血红素 - 铜氧化还原酶。然而,铜也是有毒的,因此细胞需要一个高度协调的铜摄取和传递系统来防止有毒铜浓度的积累。在本研究中,我们分析了铜传递到荚膜红细菌的cbb3型细胞色素c氧化酶(cbb3 - Cox)的过程。我们鉴定了PCuA C样周质伴侣蛋白PccA,并分析了其对cbb3 - Cox组装的贡献。我们的数据表明,PccA是一种优先结合Cu(I)的铜结合蛋白,对于高效的cbb3 - Cox组装是必需的,特别是在低铜浓度下。通过体内和体外交联,我们表明PccA与Sco1同源物SenC形成复合物。在缺乏cbb3 - Cox特异性组装因子CcoGHIS的情况下,这种复合物得以稳定。在缺乏SenC的细胞中,细胞质铜含量显著增加,但同时缺乏PccA可防止这种铜积累。这些数据表明,PccA和SenC之间的相互作用不仅在cbb3 - Cox组装过程中是铜传递所必需的,而且还调节荚膜红细菌中的铜稳态。

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