Department of Biochemistry, University of Toronto, Toronto, Ontario M5S 1A8, Canada.
Program in Molecular Medicine, Hospital for Sick Children, Toronto, Ontario M5G 1X8, Canada.
J Am Chem Soc. 2020 Dec 9;142(49):20519-20523. doi: 10.1021/jacs.0c09474. Epub 2020 Nov 24.
ClpPs are a conserved family of serine proteases that collaborate with ATP-dependent translocases to degrade protein substrates. Drugs targeting these enzymes have attracted interest for the treatment of cancer and bacterial infections due to their critical role in mitochondrial and bacterial proteostasis, respectively. As such, there is significant interest in understanding structure-function relationships in this protein family. ClpPs are known to crystallize in extended, compact, and compressed forms; however, it is unclear what conditions favor the formation of each form and whether they are populated by wild-type enzymes in solution. Here, we use cryo-EM and solution NMR spectroscopy to demonstrate that a pH-dependent conformational switch controls an equilibrium between the active extended and inactive compressed forms of ClpP from the Gram-negative pathogen . Our findings provide insight into how ClpPs exploit their rugged energy landscapes to enable key conformational changes that regulate their function.
ClpP 是一个保守的丝氨酸蛋白酶家族,与 ATP 依赖性转运体协同作用,降解蛋白质底物。由于它们在线粒体和细菌蛋白质稳态中分别具有关键作用,因此靶向这些酶的药物因其在治疗癌症和细菌感染方面的潜力而引起了人们的关注。因此,人们对理解该蛋白质家族的结构-功能关系非常感兴趣。ClpP 已知以扩展、紧凑和压缩形式结晶;然而,目前尚不清楚哪种条件有利于每种形式的形成,以及它们是否在溶液中由野生型酶占据。在这里,我们使用 cryo-EM 和溶液 NMR 光谱学来证明 pH 依赖性构象转换控制革兰氏阴性病原体的 ClpP 的活性扩展形式和非活性压缩形式之间的平衡。我们的发现为 ClpP 如何利用其崎岖的能量景观来实现调节其功能的关键构象变化提供了深入了解。
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