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Cargo engagement protects protease adaptors from degradation in a substrate-specific manner

机译:货物结合可以保护蛋白酶接头免于以底物特异性方式降解

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摘要

Protein degradation in bacteria is a highly controlled process involving proteolytic adaptors that regulate protein degradation during cell cycle progression or during stress responses. Many adaptors work as scaffolds that selectively bind cargo and tether substrates to their cognate proteases to promote substrate destruction, whereas others primarily activate the target protease. Because adaptors must bind their cognate protease, all adaptors run the risk of being recognized by the protease as substrates themselves, a process that could limit their effectiveness. Here we use purified proteins in a reconstituted system and in vivo studies to show that adaptors of the ClpXP protease are readily degraded but that cargo binding inhibits this degradation. We found that this principle extends across several adaptor systems, including the hierarchical adaptors that drive the Caulobacter bacterial cell cycle and the quality control adaptor SspB. We also found that the ability of a cargo to protect its adaptor is adaptor substrate-specific, as adaptors with artificial degradation tags were not protected even though cargo binding is unaffected. Our work points to an optimization of inherent adaptor degradation and cargo binding that ensures that robust adaptor activity is maintained when high amounts of substrate must be delivered and that adaptors can be eliminated when their tasks have been completed.
机译:细菌中的蛋白质降解是一个高度受控的过程,涉及蛋白水解适配器,该适配器在细胞周期进程或应激反应期间调节蛋白质降解。许多衔接子充当支架,可选择性地将货物和系链底物与其同源蛋白酶结合,以促进底物破坏,而其他衔接子则主要激活靶蛋白酶。由于衔接子必须结合其同源蛋白酶,因此所有衔接子都有被蛋白酶识别为底物本身的风险,该过程可能会限制其有效性。在这里,我们在重组系统和体内研究中使用纯化的蛋白质,以显示ClpXP蛋白酶的衔接子易于降解,但货物结合抑制了这种降解。我们发现,该原理遍及多个适配器系统,包括驱动杆状细菌细菌细胞周期的分层适配器和质量控制适配器SspB。我们还发现,货物保护其适配器的能力是适配器特定于适配器的,这是因为即使货物绑定不受影响,带有人工降解标签的适配器也没有受到保护。我们的工作针对固有适配器的退化和货物绑定进行了优化,以确保当必须交付大量基材时可以保持强大的适配器活动,并在完成任务后可以消除适配器。

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