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与β-桶组装机器的核心组件BamA的周质结构域片段结合的BamB的晶体结构。

Crystal structure of BamB bound to a periplasmic domain fragment of BamA, the central component of the β-barrel assembly machine.

作者信息

Jansen Katarina Bartoš, Baker Susan Lynn, Sousa Marcelo Carlos

机构信息

From the Department of Chemistry and Biochemistry, University of Colorado, Boulder, Colorado 80309.

From the Department of Chemistry and Biochemistry, University of Colorado, Boulder, Colorado 80309

出版信息

J Biol Chem. 2015 Jan 23;290(4):2126-36. doi: 10.1074/jbc.M114.584524. Epub 2014 Dec 2.

Abstract

The β-barrel assembly machinery (BAM) mediates folding and insertion of β-barrel outer membrane proteins (OMPs) into the outer membrane of Gram-negative bacteria. BAM is a five-protein complex consisting of the β-barrel OMP BamA and lipoproteins BamB, -C, -D, and -E. High resolution structures of all the individual BAM subunits and a BamD-BamC complex have been determined. However, the overall complex architecture remains elusive. BamA is the central component of BAM and consists of a membrane-embedded β-barrel and a periplasmic domain with five polypeptide translocation-associated (POTRA) motifs thought to interact with the accessory lipoproteins. Here we report the crystal structure of a fusion between BamB and a POTRA3-5 fragment of BamA. Extended loops 13 and 17 protruding from one end of the BamB β-propeller contact the face of the POTRA3 β-sheet in BamA. The interface is stabilized by several hydrophobic contacts, a network of hydrogen bonds, and a cation-π interaction between BamA Tyr-255 and BamB Arg-195. Disruption of BamA-BamB binding by BamA Y255A and probing of the interface by disulfide bond cross-linking validate the physiological relevance of the observed interface. Furthermore, the structure is consistent with previously published mutagenesis studies. The periplasmic five-POTRA domain of BamA is flexible in solution due to hinge motions in the POTRA2-3 linker. Modeling BamB in complex with full-length BamA shows BamB binding at the POTRA2-3 hinge, suggesting a role in modulation of BamA flexibility and the conformational changes associated with OMP folding and insertion.

摘要

β桶组装机器(BAM)介导β桶外膜蛋白(OMP)折叠并插入革兰氏阴性菌的外膜。BAM是一种由β桶OMP BamA以及脂蛋白BamB、-C、-D和-E组成的五蛋白复合物。已确定了所有单个BAM亚基以及BamD-BamC复合物的高分辨率结构。然而,整体复合物结构仍不清楚。BamA是BAM的核心成分,由一个膜嵌入β桶和一个周质结构域组成,该周质结构域有五个与多肽转运相关(POTRA)基序,被认为与辅助脂蛋白相互作用。在此,我们报道了BamB与BamA的POTRA3-5片段融合体的晶体结构。从BamBβ螺旋桨一端伸出的延伸环13和17与BamA中POTRA3β折叠片层的表面接触。该界面通过几个疏水接触、氢键网络以及BamA的Tyr-255与BamB的Arg-195之间的阳离子-π相互作用得以稳定。通过BamA Y255A破坏BamA-BamB结合以及通过二硫键交联探测该界面,验证了所观察到的界面的生理相关性。此外,该结构与先前发表的诱变研究一致。由于POTRA2-3连接子中的铰链运动,BamA的周质五POTRA结构域在溶液中具有柔性。对与全长BamA形成复合物的BamB进行建模显示,BamB在POTRA2-3铰链处结合,表明其在调节BamA柔性以及与OMP折叠和插入相关的构象变化中发挥作用。

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