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大肠杆菌 CcdB_G100T 毒素与其同源抗毒素 CcdA 的毒素结合 C 末端结构域复合物的骨架原子指派。

Backbone assignment of CcdB_G100T toxin from E.coli in complex with the toxin binding C-terminal domain of its cognate antitoxin CcdA.

机构信息

Molecular Biophysics Unit, Indian Institute of Science, Bengaluru, Karnataka, 560012, India.

出版信息

Biomol NMR Assign. 2024 Dec;18(2):285-292. doi: 10.1007/s12104-024-10201-6. Epub 2024 Sep 14.

Abstract

The CcdAB system expressed in the E.coli cells is a prototypical example of the bacterial toxin-antitoxin (TA) systems that ensure the survival of the bacterial population under adverse environmental conditions. The solution and crystal structures of CcdA, CcdB and of CcdB in complex with the toxin-binding C-terminal domain of CcdA have been reported. Our interest lies in the dynamics of CcdB-CcdA complex formation. Solution NMR studies have shown that CcdB_G100T, in presence of saturating concentrations of CcdA-c, a truncated C-terminal fragment of CcdA exists in equilibrium between two major populations. Sequence specific backbone resonance assignments of both equilibrium forms of the ~ 27 kDa complex, have been obtained from a suite of triple resonance NMR experiments acquired on H, C, N enriched samples of CcdB_G100T. Analysis of H, C, C secondary chemical shifts, shows that both equilibrium forms of CcdB_G100T have five beta-strands and one alpha-helix as the major secondary structural elements in the tertiary structure. The results of these studies are presented below.

摘要

在大肠杆菌细胞中表达的 CcdAB 系统是细菌毒素-抗毒素(TA)系统的典型范例,该系统可确保细菌种群在不利的环境条件下生存。已报道了 CcdA、CcdB 和 CcdB 与 CcdA 的毒素结合 C 末端结构域复合物的溶液和晶体结构。我们的兴趣在于 CcdB-CcdA 复合物形成的动力学。溶液 NMR 研究表明,在 CcdA-c(CcdA 的截短 C 末端片段)的饱和浓度存在下,CcdB_G100T 存在于两种主要群体之间的平衡。通过在 H、C、N 富集的 CcdB_G100T 样品上进行的一系列三共振 NMR 实验,获得了 ~27 kDa 复合物两种平衡形式的序列特异性骨架共振分配。对 H、C、C 二级化学位移的分析表明,CcdB_G100T 的两种平衡形式在三级结构中均具有五个β-链和一个α-螺旋作为主要二级结构元件。以下呈现这些研究的结果。

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