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长程动态相关调控细菌酪氨酸激酶 Wzc 的催化活性。

Long-range dynamic correlations regulate the catalytic activity of the bacterial tyrosine kinase Wzc.

机构信息

Department of Chemistry and Biochemistry, The City College of New York, New York, NY 10031, USA.

PhD Program in Biochemistry, The Graduate Center of CUNY, New York, NY 10016, USA.

出版信息

Sci Adv. 2020 Dec 18;6(51). doi: 10.1126/sciadv.abd3718. Print 2020 Dec.

Abstract

BY-kinases represent a highly conserved family of protein tyrosine kinases unique to bacteria without eukaryotic orthologs. BY-kinases are regulated by oligomerization-enabled transphosphorylation on a C-terminal tyrosine cluster through a process with sparse mechanistic detail. Using the catalytic domain (CD) of the archetypal BY-kinase, Wzc, and enhanced-sampling molecular dynamics simulations, isothermal titration calorimetry and nuclear magnetic resonance measurements, we propose a mechanism for its activation and nucleotide exchange. We find that the monomeric Wzc CD preferentially populates states characterized by distortions at its oligomerization interfaces and by catalytic element conformations that allow high-affinity interactions with ADP but not with ATP·Mg We propose that oligomer formation stabilizes the intermonomer interfaces and results in catalytic element conformations suitable for optimally engaging ATP·Mg, facilitating exchange with bound ADP. This sequence of events, oligomerization, i.e., substrate binding, before engaging ATP·Mg, facilitates optimal autophosphorylation by preventing a futile cycle of ATP hydrolysis.

摘要

BY-kinases 是一种高度保守的蛋白酪氨酸激酶家族,仅存在于细菌中,而在真核生物中没有同源物。BY-kinases 通过一个机制细节稀疏的寡聚化促进的 C 末端酪氨酸簇的转磷酸化过程进行调节。使用典型的 BY-kinase Wzc 的催化结构域 (CD) 和增强采样分子动力学模拟、等温滴定量热法和核磁共振测量,我们提出了其激活和核苷酸交换的机制。我们发现单体 Wzc CD 优先分布在其寡聚化界面发生扭曲和催化元件构象的状态,这些构象允许与 ADP 高亲和力相互作用,但与 ATP·Mg 不相互作用。我们提出寡聚体形成稳定了互变异构体界面,并导致适合与 ATP·Mg 最佳结合的催化元件构象,从而促进与结合的 ADP 的交换。这一系列事件,即寡聚化,即底物结合,在与 ATP·Mg 结合之前,通过防止无效的 ATP 水解循环,促进了最佳的自磷酸化。

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