首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Structural basis for the allosteric control of the global transcription factor NtcA by the nitrogen starvation signal 2-oxoglutarate
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Structural basis for the allosteric control of the global transcription factor NtcA by the nitrogen starvation signal 2-oxoglutarate

机译:氮饥饿信号2-氧戊二酸对全局转录因子NtcA的变构控制的结构基础

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摘要

2-oxogluatarate (2-OG), a metabolite of the highly conserved Krebs cycle, not only plays a critical role in metabolism, but also constitutes a signaling molecule in a variety of organisms ranging from bacteria to plants and animals. In cyanobacteria, the accumulation of 2-OG constitutes the signal of nitrogen starvation and NtcA, a global transcription factor, has been proposed as a putative receptor for 2-OG. Here we present three crystal structures of NtcA from the cyanobacterium Anabaena: the apoform, and two ligand-bound forms in complex with either 2-OG or its analogue 2,2-difluoropentanedioic acid. All structures assemble as homodimers, with each subunit composed of an N-terminal effector-binding domain and a C-terminal DNA-binding domain connected by a long helix (C-helix). The 2-OG binds to the effector-binding domain at a pocket similar to that used by cAMP in catabolite activator protein, but with a different pattern. Comparative structural analysis reveals a putative signal transmission route upon 2-OG binding. A tighter coiled-coil conformation of the two C-helices induced by 2-OG is crucial to maintain the proper distance between the two F-helices for DNA recognition. Whereas catabolite activator protein adopts a transition from off-to-on state upon cAMP binding, our structural analysis explains well why NtcA can bind to DNA even in its apoform, and how 2-OG just enhances the DNA-binding activity of NtcA. These findings provided the structural insights into the function of a global transcription factor regulated by 2-OG, a metabolite standing at a crossroad between carbon and nitrogen metabolisms.
机译:2-氧杂戊酸(2-OG)是高度保守的克雷布斯循环的代谢产物,不仅在代谢中起关键作用,而且还构成了从细菌到动植物的各种生物的信号分子。在蓝细菌中,2-OG的积累构成了氮饥饿的信号,并且已经提出了一种全球转录因子NtcA作为2-OG的假定受体。在这里,我们介绍了来自蓝细菌鱼腥藻的NtcA的三个晶体结构:脱辅基,以及两个与2-OG或其类似物2,2-二氟戊二酸复合的配体结合形式。所有结构组装成同型二聚体,每个亚基由一个长螺旋(C螺旋)连接的一个N末端效应子结合结构域和一个C末端DNA结合结构域组成。 2-OG在与分解代谢活化蛋白中的cAMP相似的口袋处与效应子结合结构域结合,但模式不同。比较结构分析揭示了2-OG结合后的假定信号传输途径。 2-OG诱导的两个C螺旋的紧密盘绕构象对于保持两个F螺旋之间的适当距离对于DNA识别至关重要。分解代谢物激活蛋白在cAMP结合后从关闭状态转变为打开状态,而我们的结构分析很好地解释了为什么NtcA甚至可以在其apoform中也能与DNA结合,以及2-OG如何增强NtcA的DNA结合活性。这些发现为2-OG调节的全局转录因子的功能提供了结构上的见识,2-OG是站在碳和氮代谢之间的十字路口的代谢产物。

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