首页> 美国卫生研究院文献>The Journal of Biological Chemistry >Repetitive Protein Unfolding by the trans Ring of the GroEL-GroES Chaperonin Complex Stimulates Folding
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Repetitive Protein Unfolding by the trans Ring of the GroEL-GroES Chaperonin Complex Stimulates Folding

机译:GroEL-GroES伴侣蛋白复合物的反式环重复蛋白质解折叠刺激折叠。

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摘要

A key constraint on the growth of most organisms is the slow and inefficient folding of many essential proteins. To deal with this problem, several diverse families of protein folding machines, known collectively as molecular chaperones, developed early in evolutionary history. The functional role and operational steps of these remarkably complex nanomachines remain subjects of active debate. Here we present evidence that, for the GroEL-GroES chaperonin system, the non-native substrate protein enters the folding cycle on the trans ring of the double-ring GroEL-ATP-GroES complex rather than the ADP-bound complex. The properties of this ATP complex are designed to ensure that non-native substrate protein binds first, followed by ATP and finally GroES. This binding order ensures efficient occupancy of the open GroEL ring and allows for disruption of misfolded structures through two phases of multiaxis unfolding. In this model, repeated cycles of partial unfolding, followed by confinement within the GroEL-GroES chamber, provide the most effective overall mechanism for facilitating the folding of the most stringently dependent GroEL substrate proteins.
机译:大多数生物生长的关键限制因素是许多必需蛋白质的缓慢折叠和无效折叠。为了解决这个问题,在进化历史的早期发展了几种不同的蛋白质折叠机家族,统称为分子伴侣。这些非常复杂的纳米机器的功能作用和操作步骤仍然是人们争论的焦点。在这里,我们提供的证据表明,对于GroEL-GroES伴侣蛋白系统,非天然底物蛋白进入双环GroEL-ATP-GroES复合物而不是与ADP结合的复合物的环上的折叠循环。设计该ATP复合物的特性以确保首先结合非天然底物蛋白,然后结合ATP,最后结合GroES。该结合顺序确保了开放式GroEL环的有效占据,并允许通过多轴展开的两个阶段破坏错折叠的结构。在此模型中,部分展开的重复循环,然后限制在GroEL-GroES腔室内,为促进最严格依赖的GroEL底物蛋白质的折叠提供了最有效的整体机制。

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