转移酶
信号转导衔接蛋白
苏氨酸
机制(生物学)
化学
糖基化
磷酸化
生物化学
计算生物学
生物物理学
丝氨酸
生物
酶
物理
量子力学
作者
Yu Wang,Zhiyang Zhang,Xiaoyuan Liu,Nianhang Chen,Yuan Zhao,Chaojie Wang
摘要
O-N-Acetylglucosamine transferase (OGT) can catalyze the O-GlcNAc modification of thousands of proteins. The holoenzyme formation of OGT and adaptor protein is the precondition for further recognition and glycosylation of the target protein, while the corresponding mechanism is still open. Here, static and dynamic schemes based on statistics can successfully screen the feasible identifying, approaching, and binding mechanism of OGT and its typical adaptor protein p38α. The most favorable interface, energy contribution of hotspots, and conformational changes of fragments were discovered. The hydrogen bond interactions were verified as the main driving force for the whole process. The distinct characteristic of active and inactive p38α is explored and demonstrates that the phosphorylated tyrosine and threonine will form strong ion-pair interactions with Lys714, playing a key role in the dynamic identification stage. Multiple method combinations from different points of view may be helpful for exploring other systems of the protein-protein interactions.
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