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Crystal structure of a soluble form of human monoglyceride lipase in complex with an inhibitor at 1.35 Å resolution

机译:可溶性形式的人甘油单酯脂肪酶与1.35Å分辨率的抑制剂形成复合物的晶体结构

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摘要

A high-resolution structure of a ligand-bound, soluble form of human monoglyceride lipase (MGL) is presented. The structure highlights a novel conformation of the regulatory lid-domain present in the lipase family as well as the binding mode of a pharmaceutically relevant reversible inhibitor. Analysis of the structure lacking the inhibitor indicates that the closed conformation can accommodate the native substrate 2-arachidonoyl glycerol. A model is proposed in which MGL undergoes conformational and electrostatic changes during the catalytic cycle ultimately resulting in its dissociation from the membrane upon completion of the cycle. In addition, the study outlines a successful approach to transform membrane associated proteins, which tend to aggregate upon purification, into a monomeric and soluble form.
机译:提出了人甘油单酯脂肪酶(MGL)的配体结合的可溶形式的高分辨率结构。该结构突出了脂肪酶家族中存在的调节性盖结构域的新构型以及药学相关可逆抑制剂的结合模式。对缺乏抑制剂的结构的分析表明,闭合构象可以容纳天然底物2-花生四烯酰基甘油。提出了一种模型,其中MGL在催化循环过程中经历构象和静电变化,最终在循环完成时导致其从膜上解离。此外,研究概述了将膜相关蛋白(纯化后趋于聚集)转化为单体和可溶形式的成功方法。

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