首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >STRUCTURE DETERMINATION OF MURINE MITOCHONDRIAL CARBONIC ANHYDRASE V AT 2.45-ANGSTROM RESOLUTION - IMPLICATIONS FOR CATALYTIC PROTON TRANSFER AND INHIBITOR DESIGN
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STRUCTURE DETERMINATION OF MURINE MITOCHONDRIAL CARBONIC ANHYDRASE V AT 2.45-ANGSTROM RESOLUTION - IMPLICATIONS FOR CATALYTIC PROTON TRANSFER AND INHIBITOR DESIGN

机译:在2.45埃分辨率下测定鼠线粒体碳酸酐酶V的结构-催化质子转移和抑制剂设计的意义

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摘要

The three-dimensional structure of murine mitochondrial carbonic anhydrase V has been determined and refined at 2.45-Angstrom resolution (crystallographic R factor = 0.187), Significant structural differences unique to the active site of carbonic anhydrase V are responsible for differences in the mechanism of catalytic proton transfer as compared with other carbonic anhydrase isozymes. In the prototypical isozyme, carbonic anhydrase II, catalytic proton transfer occurs via the shuttle group His-64; carbonic anhydrase V has Tyr-64, which is not an efficient proton shuttle due in part to the bulky adjacent side chain of Phe-65. Based on analysis of the structure of carbonic anhydrase V, we speculate that Tyr-131 may participate in proton transfer due to its proximity to zinc-bound solvent, its solvent accessibility, and its electrostatic environment in the protein structure. Finally, the design of isozyme-specific inhibitors is discussed in view of the complex between carbonic anhydrase V and acetazolamide, a transition-state analogue, Such inhibitors may be physiologically important in the regulation of blood glucose levels. [References: 45]
机译:小鼠线粒体碳酸酐酶V的三维结构已确定并以2.45埃的分辨率精制(晶体学R因子= 0.187),碳酸酐酶V活性位点独有的显着结构差异是造成催化机理的差异的原因。与其他碳酸酐酶同工酶相比,质子转移。在典型的同工酶碳酸酐酶II中,催化质子转移通过穿梭基团His-64发生。碳酸酐酶V具有Tyr-64,这不是有效的质子穿梭,部分原因是Phe-65的相邻侧链很大。基于对碳酸酐酶V结构的分析,我们推测Tyr-131可能由于其与锌结合溶剂的接近程度,其溶剂可及性以及蛋白质结构中的静电环境而参与质子转移。最后,鉴于碳酸酐酶V和乙酰唑胺(过渡态类似物)之间的复杂性,讨论了同工酶特异性抑制剂的设计。此类抑制剂在调节血糖水平方面可能具有重要的生理意义。 [参考:45]

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