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HAMP结构域在细菌化学感受器趋化信号传导中的作用。

Role of HAMP domains in chemotaxis signaling by bacterial chemoreceptors.

作者信息

Khursigara Cezar M, Wu Xiongwu, Zhang Peijun, Lefman Jonathan, Subramaniam Sriram

机构信息

Laboratory of Cell Biology, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

Proc Natl Acad Sci U S A. 2008 Oct 28;105(43):16555-60. doi: 10.1073/pnas.0806401105. Epub 2008 Oct 21.

Abstract

Bacterial chemoreceptors undergo conformational changes in response to variations in the concentration of extracellular ligands. These changes in chemoreceptor structure initiate a series of signaling events that ultimately result in regulation of rotation of the flagellar motor. Here we have used cryo-electron tomography combined with 3D averaging to determine the in situ structure of chemoreceptor assemblies in Escherichia coli cells that have been engineered to overproduce the serine chemoreceptor Tsr. We demonstrate that chemoreceptors are organized as trimers of receptor dimers and display two distinct conformations that differ principally in arrangement of the HAMP domains within each trimer. Ligand binding and methylation alter the distribution of chemoreceptors between the two conformations, with serine binding favoring the "expanded" conformation and chemoreceptor methylation favoring the "compact" conformation. The distinct positions of chemoreceptor HAMP domains within the context of a trimeric unit are thus likely to represent important aspects of chemoreceptor structural changes relevant to chemotaxis signaling. Based on these results, we propose that the compact and expanded conformations represent the "kinase-on" and "kinase-off" states of chemoreceptor trimers, respectively.

摘要

细菌化学感受器会根据细胞外配体浓度的变化发生构象变化。化学感受器结构的这些变化引发一系列信号事件,最终导致鞭毛马达旋转的调节。在此,我们使用冷冻电子断层扫描结合三维平均技术来确定经工程改造以过量表达丝氨酸化学感受器Tsr的大肠杆菌细胞中化学感受器组装体的原位结构。我们证明,化学感受器以受体二聚体的三聚体形式组织,并呈现出两种不同的构象,主要区别在于每个三聚体内HAMP结构域的排列方式。配体结合和甲基化改变了化学感受器在两种构象之间的分布,丝氨酸结合有利于“扩展”构象,而化学感受器甲基化有利于“紧凑”构象。因此,在三聚体单元背景下化学感受器HAMP结构域的不同位置可能代表了与趋化信号相关的化学感受器结构变化的重要方面。基于这些结果,我们提出紧凑构象和扩展构象分别代表化学感受器三聚体的“激酶开启”和“激酶关闭”状态。

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