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首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Lethal factor unfolding is the most force-dependent step of anthrax toxin translocation
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Lethal factor unfolding is the most force-dependent step of anthrax toxin translocation

机译:致死因子的展开是炭疽毒素易位的最受力依赖的步骤

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Cellular compartmentalization requires machinery capable of translocating polypeptides across membranes. In many cases, transported proteins must first be unfolded by means of the proton motive force and/or ATP hydrolysis. Anthrax toxin, which is composed of a channel-forming protein and two substrate proteins, is an attractive model system to study translocation-coupled unfolding, because the applied driving force can be externally controlled and translocation can be monitored directly by using electrophys-iology. By controlling the driving force and introducing destabilizing point mutations in the substrate, we identified the barriers in the transport pathway, determined which barrier corresponds to protein unfolding, and mapped how the substrate protein unfolds during translocation. In contrast to previous studies, we find that the protein's structure next to the signal tag is not rate-limiting to unfolding. Instead, a more extensive part of the structure, the amino-terminal β-sheet subdomain, must disassemble to cross the unfolding barrier. We also find that unfolding is catalyzed by the channel's phenylalanine-clamp active site. We propose a broad molecular mechanism for translocation-coupled unfolding, which is applicable to both soluble and membrane-embedded unfolding machines.
机译:细胞区室化需要能够跨膜转运多肽的机制。在许多情况下,必须首先借助质子原动力和/或ATP水解使转运的蛋白质解折叠。炭疽毒素由通道形成蛋白和两个底物蛋白组成,是研究转运耦合展开的一种有吸引力的模型系统,因为所施加的驱动力可以从外部进行控制并且可以通过电生理学直接监测转运。通过控制驱动力并在底物中引入破坏稳定点的突变,我们确定了运输途径中的障碍,确定了哪个障碍对应于蛋白质的解折叠,并绘制了在转运过程中底物蛋白质如何展开的图。与以前的研究相比,我们发现信号标签旁边的蛋白质结构不限速。取而代之的是,该结构的更广泛的部分,即氨基末端β-sheet亚结构域,必须分解才能穿过展开的屏障。我们还发现,通道的苯丙氨酸钳位活性位点催化了展开。我们提出了一个易位偶联展开的广泛分子机制,这适用于可溶和膜嵌入的展开机。

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