首页> 外文期刊>Journal of Molecular Biology >Stepwise unfolding of a beta barrel protein by the AAA+ ClpXP protease.
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Stepwise unfolding of a beta barrel protein by the AAA+ ClpXP protease.

机译:AAA + ClpXP蛋白酶逐步展开β桶蛋白。

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In the AAA+ ClpXP protease, ClpX uses the energy of ATP binding and hydrolysis to unfold proteins before translocating them into ClpP for degradation. For proteins with C-terminal ssrA tags, ClpXP pulls on the tag to initiate unfolding and subsequent degradation. Here, we demonstrate that an initial step in ClpXP unfolding of the 11-stranded beta barrel of superfolder GFP-ssrA involves extraction of the C-terminal beta strand. The resulting 10-stranded intermediate is populated at low ATP concentrations, which stall ClpXP unfolding, and at high ATP concentrations, which support robust degradation. To determine if stable unfolding intermediates cause low-ATP stalling, we designed and characterized circularly permuted GFP variants. Notably, stalling was observed for a variant that formed a stable 10-stranded intermediate but not for one in which this intermediate was unstable. A stepwise degradation model in which the rates of terminal-strand extraction, strand refolding or recapture, and unfolding of the 10-stranded intermediate all depend on the rate of ATP hydrolysis by ClpXP accounts for the observed changes in degradation kinetics over a broad range of ATP concentrations. Our results suggest that the presence or absence of unfolding intermediates will play important roles in determining whether forced enzymatic unfolding requires a minimum rate of ATP hydrolysis.
机译:在AAA + ClpXP蛋白酶中,ClpX利用ATP结合和水解的能量来展开蛋白质,然后再将它们转移到ClpP中进行降解。对于具有C端ssrA标签的蛋白质,ClpXP会拉紧标签以启动展开并随后降解。在这里,我们证明了ClpXP展开的超级文件夹GFP-ssrA的11链β桶的起始步骤涉及C末端β链的提取。所得的10链中间体在低ATP浓度(阻止ClpXP展开)和高ATP浓度(支持鲁棒降解)的条件下填充。为了确定稳定的展开中间体是否会导致低ATP失速,我们设计并鉴定了圆形排列的GFP变体。值得注意的是,对于形成稳定的10链中间体的变体观察到失速,但是对于该中间体不稳定的变体则没有观察到失速。逐步降解模型,其中末端链的提取,链重折叠或重新捕获以及10链中间体的解折叠速率均取决于ClpXP的ATP水解速率,这说明了观察到的降解动力学变化范围很大。 ATP浓度。我们的结果表明,存在或不存在的中间体中间体将在确定强制酶解是否需要最小的ATP水解速率方面发挥重要作用。

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