首页> 美国卫生研究院文献>Acta Crystallographica Section F: Structural Biology and Crystallization Communications >Structure of human glycolate oxidase in complex with the inhibitor 4-carboxy-5-(4-chlorophenyl)sulfanyl-123-thiadiazole
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Structure of human glycolate oxidase in complex with the inhibitor 4-carboxy-5-(4-chlorophenyl)sulfanyl-123-thiadiazole

机译:人乙醇酸氧化酶与抑制剂4-羧基-5-(4-氯苯基)硫烷基 -123-噻二唑配合物的结构

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摘要

Glycolate oxidase, a peroxisomal flavoenzyme, generates glyoxylate at the expense of oxygen. When the normal metabolism of glyoxylate is impaired by the mutations that are responsible for the genetic diseases hyperoxaluria types 1 and 2, glyoxylate yields oxalate, which forms insoluble calcium deposits, particularly in the kidneys. Glycolate oxidase could thus be an interesting therapeutic target. The crystal structure of human glycolate oxidase (hGOX) in complex with 4-carboxy-5-[(4-chlorophenyl)sulfanyl]-1,2,3-thiadiazole (CCPST) has been determined at 2.8 Å resolution. The inhibitor heteroatoms interact with five active-site residues that have been implicated in catalysis in homologous flavodehydrogenases of l-2-hydroxy acids. In addition, the chlorophenyl substituent is surrounded by nonconserved hydrophobic residues. The present study highlights the role of mobility in ligand binding by glycolate oxidase. In addition, it pinpoints several structural differences between members of the highly conserved family of flavodehydrogenases of l-2-hydroxy acids.
机译:乙醛酸氧化酶,一种过氧化物酶体黄酮酶,以氧气为代价产生乙醛酸。当乙醛酸酯的正常代谢受到遗传性疾病1和2型高草酸尿症的突变的影响时,乙醛酸酯会产生草酸,形成不可溶的钙沉积物,特别是在肾脏中。因此,乙醇酸氧化酶可能是有趣的治疗靶标。已确定人乙醇酸氧化酶(hGOX)与4-羧基-5-[(4-氯苯基)硫烷基] -1,2,3-噻二唑(CCPST)的晶体结构为2.8?Å分辨率。抑制剂杂原子与5个活性位点残基相互作用,这些残基已牵涉到L-2-羟基酸的同源黄酮脱氢酶的催化作用中。另外,氯苯基取代基被非保守的疏水残基包围。本研究强调了乙醇酸氧化酶在配体结合中迁移的作用。此外,它指出了1-2羟基酸黄酮脱氢酶的高度保守家族成员之间的几个结构差异。

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