School of Life Science, Gwangju Institute of Science & Technology (GIST), Gwangju 500-712, Korea.
Mol Microbiol. 2010 Jun 1;76(5):1222-31. doi: 10.1111/j.1365-2958.2010.07160.x. Epub 2010 Apr 14.
In Gram-negative bacteria, proper placement of the FtsZ ring, mediated by nucleoid occlusion and the activities of the dynamic oscillating Min proteins MinC, MinD and MinE, is required for correct positioning of the cell division septum. MinE is a topological specificity factor that counters the activity of MinCD division inhibitor at the mid-cell division site. Its structure consists of an anti-MinCD domain and a topology specificity domain (TSD). Previous NMR analysis of truncated Escherichia coli MinE showed that the TSD domain contains a long alpha-helix and two anti-parallel beta-strands, which mediate formation of a homodimeric alpha/beta structure. Here we report the crystal structure of full-length Helicobacter pylori MinE and redefine its TSD based on that structure. The N-terminal region of the TSD (residues 19-26), previously defined as part of the anti-MinCD domain, forms a beta-strand (betaA) and participates in TSD folding. In addition, H. pylori MinE forms a dimer through the interaction of anti-parallel betaA-strands. Moreover, we observed serial dimer-dimer interactions within the crystal packing, resulting in the formation of a multimeric structure. We therefore redefine the functional domain of MinE and propose that a multimeric filamentous structure is formed through anti-parallel beta-strand interactions.
在革兰氏阴性细菌中,FtsZ 环的正确定位,通过核区封闭和动态振荡 Min 蛋白 MinC、MinD 和 MinE 的活性来介导,是正确定位细胞分裂隔膜所必需的。MinE 是拓扑特异性因子,可对抗在细胞中部分裂位点的 MinCD 分裂抑制剂的活性。它的结构由一个抗 MinCD 结构域和一个拓扑特异性结构域(TSD)组成。以前对截断的大肠杆菌 MinE 的 NMR 分析表明,TSD 结构域包含一个长的α-螺旋和两个反平行的β-折叠,介导同源二聚体α/β结构的形成。在这里,我们报告了完整的幽门螺杆菌 MinE 的晶体结构,并根据该结构重新定义了其 TSD。TSD 的 N 端区域(残基 19-26),以前被定义为抗 MinCD 结构域的一部分,形成一个β-折叠(βA)并参与 TSD 折叠。此外,幽门螺杆菌 MinE 通过反平行的βA-链相互作用形成二聚体。此外,我们在晶体包装中观察到一系列的二聚体-二聚体相互作用,导致形成多聚体结构。因此,我们重新定义了 MinE 的功能域,并提出通过反平行的β-折叠相互作用形成多聚体丝状结构。
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