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A novel partially open state of SHP2 points to a multiple gear regulation mechanism

机译:SHP2的新型开放状态指向多齿轮调节机构

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摘要

The protein tyrosine phosphatase SHP2 mediates multiple signal transductions in various cellular pathways, controlled by a variety of upstream inputs. SHP2 dysregulation is causative of different types of cancers and developmental disorders, making it a promising drug target. However, how SHP2 is modulated by its different regulators remains largely unknown. Here, we use single-molecule fluorescence resonance energy transfer and molecular dynamics simulations to investigate this question. We identify a partially open, semiactive conformation of SHP2 that is intermediate between the known open and closed states. We further demonstrate a “multiple gear” regulatory mechanism, in which different activators (e.g., insulin receptor substrate-1 and CagA), oncogenic mutations (e.g., E76A), and allosteric inhibitors (e.g., SHP099) can shift the equilibrium of the three conformational states and regulate SHP2 activity to different levels. Our work reveals the essential role of the intermediate state in fine-tuning the activity of SHP2, which may provide new opportunities for drug development for relevant cancers.
机译:蛋白酪氨酸磷酸酶SHP2介导多种蜂窝途径中的多个信号转导,由各种上游输入控制。 SHP2失呼算法是造成不同类型的癌症和发育障碍,使其成为有前途的药物目标。但是,SHP2如何由其不同的调节器调制仍然很大程度上是未知的。在这里,我们使用单分子荧光共振能量传递和分子动力学模拟来调查这个问题。我们识别出在已知的开放和封闭状态之间中间的SHP2的部分打开,半视角构象。我们进一步证明了“多齿轮”调节机制,其中不同的激活剂(例如,胰岛素受体基质-1和Caga),致癌突变(例如,E76a)和颠覆抑制剂(例如,SHP099)可以移动三个的平衡构象状态并将SHP2活动调节到不同层面。我们的工作揭示了中间国家在微调SHP2活动方面的基本作用,这可能为相关癌症提供新的药物发育机会。

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