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NADPH 耗尽的牛肝过氧化氢酶及其抑制剂复合物的结构分析。

Structural analysis of NADPH depleted bovine liver catalase and its inhibitor complexes.

作者信息

Sugadev Ragumani, Ponnuswamy M N, Sekar K

出版信息

Int J Biochem Mol Biol. 2011;2(1):67-77. Epub 2011 Jan 29.

Abstract

To study the functional role of NADPH during mammalian catalase inhibition, the X-ray crystal structures of NADPH-depleted bovine liver catalase and its inhibitor complexes, cyanide and azide, determined at 2.8Å resolution. From the complex structures it is observed that subunits with and without an inhibitor/catalytic water molecule are linked by N-terminal domain swapping. Comparing mammalian- and fungal- catalases, we speculate that NADPH-depleted mammalian catalases may function as a domain-swapped dimer of dimers, especially during inactivation by inhibitors like cyanide and azide. We further speculate that in mammalian catalases the N-terminal hinge-loop region and α-helix is the structural element that senses NADPH binding. Although the above arguments are speculative and need further verification, as a whole our studies have opened up a new possibility, viz. that mammalian catalase acts as a domain-swapped dimer of dimers, especially during inhibitor binding. To generalize this concept to the formation of the inactive state in mammalian catalases in the absence of tightly bound NADPH molecules needs further exploration. The present study adds one more intriguing fact to the existing mysteries of mammalian catalases.

摘要

为了研究NADPH在哺乳动物过氧化氢酶抑制过程中的功能作用,我们测定了在2.8Å分辨率下的NADPH缺失型牛肝过氧化氢酶及其抑制剂复合物(氰化物和叠氮化物)的X射线晶体结构。从复合物结构中观察到,有和没有抑制剂/催化水分子的亚基通过N端结构域交换相连。比较哺乳动物和真菌的过氧化氢酶,我们推测NADPH缺失的哺乳动物过氧化氢酶可能作为二聚体的结构域交换二聚体发挥作用,特别是在被氰化物和叠氮化物等抑制剂失活期间。我们进一步推测,在哺乳动物过氧化氢酶中,N端铰链环区域和α螺旋是感知NADPH结合的结构元件。尽管上述观点具有推测性,需要进一步验证,但总体而言,我们的研究开辟了一种新的可能性,即哺乳动物过氧化氢酶作为二聚体的结构域交换二聚体发挥作用,特别是在抑制剂结合期间。要将这一概念推广到在没有紧密结合的NADPH分子的情况下哺乳动物过氧化氢酶无活性状态的形成,还需要进一步探索。本研究为哺乳动物过氧化氢酶现有的谜团增添了又一个有趣的事实。

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