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基于结构的嗜热栖热菌HB8新型血红素结合蛋白的功能鉴定

Structure-based functional identification of a novel heme-binding protein from Thermus thermophilus HB8.

作者信息

Ebihara Akio, Okamoto Akihiro, Kousumi Yukihide, Yamamoto Hitoshi, Masui Ryoji, Ueyama Norikazu, Yokoyama Shigeyuki, Kuramitsu Seiki

机构信息

RIKEN Harima Institute at SPring-8, Kouto, Mikazuki-cho, Sayo-gun, Hyogo, 679-5148, Japan.

出版信息

J Struct Funct Genomics. 2005;6(1):21-32. doi: 10.1007/s10969-005-1103-x.

DOI:10.1007/s10969-005-1103-x
PMID:15965735
Abstract

The TT1485 gene from Thermus thermophilus HB8 encodes a hypothetical protein of unknown function with about 20 sequence homologs of bacterial or archaeal origin. Together they form a family of uncharacterized proteins, the cluster of orthologous group COG3253. Using a combination of amino acid sequence analysis, three-dimensional structural studies and biochemical assays, we identified TT1485 as a novel heme-binding protein. The crystal structure reveals that this protein is a pentamer and each monomer exhibits a beta-barrel fold. TT1485 is structurally similar to muconolactone isomerase, but this provided no functional clues. Amino acid sequence analysis revealed remote homology to a heme enzyme, chlorite dismutase. Strikingly, amino acid residues that are highly conserved in the homologous hypothetical proteins and chlorite dismutase cluster around a deep cavity on the surface of each monomer. Molecular modeling shows that the cavity can accommodate a heme group with a strictly conserved His as a heme ligand. TT1485 reconstituted with iron protoporphyrin IX chloride gave a low chlorite dismutase activity, indicating that TT1485 catalyzes a reaction other than chlorite degradation. The presence of a possible Fe-His-Asp triad in the heme proximal site suggests that TT1485 functions as a novel heme peroxidase to detoxify hydrogen peroxide within the cell.

摘要

嗜热栖热菌HB8的TT1485基因编码一种功能未知的假定蛋白,它与约20个细菌或古菌来源的序列同源物相关。它们共同构成了一个未表征蛋白家族,即直系同源簇COG3253。通过结合氨基酸序列分析、三维结构研究和生化分析,我们确定TT1485是一种新型血红素结合蛋白。晶体结构显示该蛋白是五聚体,每个单体呈现β桶状折叠。TT1485在结构上与粘康酸内酯异构酶相似,但这并未提供功能线索。氨基酸序列分析揭示了它与血红素酶亚氯酸盐歧化酶存在远缘同源性。引人注目的是,在同源假定蛋白和亚氯酸盐歧化酶中高度保守的氨基酸残基聚集在每个单体表面的一个深腔内。分子建模表明,该腔可以容纳一个血红素基团,其中一个严格保守的组氨酸作为血红素配体。用氯化铁原卟啉IX重构的TT1485具有较低的亚氯酸盐歧化酶活性,这表明TT148催化除亚氯酸盐降解以外的反应。血红素近端位点可能存在的铁-组氨酸-天冬氨酸三联体表明,TT1485作为一种新型血红素过氧化物酶在细胞内使过氧化氢解毒。

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