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A glutamate switch controls voltage-sensitive phosphatase function

机译:谷氨酸开关控制电压敏感磷酸酶功能

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摘要

Ciona intestinalis voltage sensing phosphatase Ci-VSP couples a voltage-sensing domain (VSD) to a lipid phosphatase similar to the tumor suppressor PTEN. How the VSD controls enzyme function has been unclear. Here, we present high-resolution crystal structures of the Ci-VSP enzymatic domain that reveal conformational changes in a key loop, termed the “gating loop”, that controls access to the active site by a mechanism in which residue Glu411 directly competes with substrate. Structure-based mutations that restrict gating loop conformation impair catalytic function and demonstrate that Glu411 also contributes to substrate selectivity. Structure-guided mutations further define an interaction between the gating loop and linker that connects the phosphatase to the VSD for voltage control of enzyme activity. Together, the data suggest that functional coupling between the gating loop and the linker forms the heart of the regulatory mechanism that controls voltage-dependent enzyme activation.
机译:Ciona intestinalis电压检测磷酸酶Ci-Vsp将电压传感结构域(VSD)致其与肿瘤抑制PTEN类似的脂质磷酸酶。 VSD控制酶功能如何尚不清楚。这里,我们呈现CI-VSP酶域的高分辨率晶体结构,其揭示关键环路中的构象变化,称为“门控环”,该机制控制对活动站点的访问,其中残留Glu411直接与基板竞争的机制。限制浇注环构象的基于结构的突变损害催化功能,并证明GLU411也有助于衬底选择性。结构引导突变进一步限定了将磷酸酶与VSD连接到VSD的接头之间的相互作用,用于酶活性的电压控制。在一起,数据表明,门控环和连接器之间的功能耦合形成控制电压依赖性酶活化的调节机制的心脏。

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