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卤代酚在脱卤过氧化物酶-血红蛋白中的内部结合抑制过氧化物酶的功能。

Internal binding of halogenated phenols in dehaloperoxidase-hemoglobin inhibits peroxidase function.

机构信息

Department of Chemistry, North Carolina State University, Raleigh, North Carolina, USA.

出版信息

Biophys J. 2010 Sep 8;99(5):1586-95. doi: 10.1016/j.bpj.2010.05.041.

Abstract

Dehaloperoxidase (DHP) from the annelid Amphitrite ornata is a catalytically active hemoglobin-peroxidase that possesses a unique internal binding cavity in the distal pocket above the heme. The previously published crystal structure of DHP shows 4-iodophenol bound internally. This led to the proposal that the internal binding site is the active site for phenol oxidation. However, the native substrate for DHP is 2,4,6-tribromophenol, and all attempts to bind 2,4,6-tribromophenol in the internal site under physiological conditions have failed. Herein, we show that the binding of 4-halophenols in the internal pocket inhibits enzymatic function. Furthermore, we demonstrate that DHP has a unique two-site competitive binding mechanism in which the internal and external binding sites communicate through two conformations of the distal histidine of the enzyme, resulting in nonclassical competitive inhibition. The same distal histidine conformations involved in DHP function regulate oxygen binding and release during transport and storage by hemoglobins and myoglobins. This work provides further support for the hypothesis that DHP possesses an external binding site for substrate oxidation, as is typical for the peroxidase family of enzymes.

摘要

脱卤过氧化物酶(DHP)来自环节动物 Amphitrite ornata,是一种具有催化活性的血红蛋白过氧化物酶,在血红素上方的远端口袋中有一个独特的内部结合腔。先前发表的 DHP 晶体结构显示 4-碘苯酚结合在内部。这导致了内部结合位点是苯酚氧化的活性位点的假设。然而,DHP 的天然底物是 2,4,6-三溴苯酚,并且在生理条件下尝试将 2,4,6-三溴苯酚结合到内部位点的所有尝试都失败了。本文中,我们表明,在内部口袋中结合 4-卤代苯酚会抑制酶的功能。此外,我们证明 DHP 具有独特的双位点竞争结合机制,其中内部和外部结合位点通过酶的远端组氨酸的两种构象进行通讯,导致非经典竞争抑制。参与 DHP 功能的相同远端组氨酸构象调节血红蛋白和肌红蛋白在运输和储存过程中的氧结合和释放。这项工作为 DHP 具有用于底物氧化的外部结合位点的假设提供了进一步的支持,这是过氧化物酶家族酶的典型特征。

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