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在突变体His-93→Gly中,用游离咪唑取代抹香鲸肌红蛋白的近端配体。

Replacement of the proximal ligand of sperm whale myoglobin with free imidazole in the mutant His-93-->Gly.

作者信息

Barrick D

机构信息

Institute of Molecular Biology, University of Oregon, Eugene 97403.

出版信息

Biochemistry. 1994 May 31;33(21):6546-54. doi: 10.1021/bi00187a023.

Abstract

The proximal bond between the iron atom of the heme group and the N epsilon of histidine F8 in myoglobin (Mb) and hemoglobin (Hb) is presumed to be an important determinant of heme binding, protein structure, and oxygen binding. Here a system is described in which the proximal ligand is provided intermolecularly by the histidine side chain mimic imidazole. The proximal ligand of sperm whale Mb is replaced with glycine (H93G) using site-directed mutagenesis. The addition of imidazole to Escherichia coli expressing this gene reconstitutes myoglobin function. H93G Mb purified in the presence of imidazole is spectroscopically similar to wild-type Mb in combination with a wide variety of distal ligands. The crystal structure of H93G Mb, determined in the presence of imidazole, reveals that an imidazole molecule is bonded to the heme iron on the proximal side, substituting in trans for the side-chain function of the proximal histidine of wild-type Mb. Although H93G Mb is similar in spectroscopic and gross structural detail to wild-type Mb, subtle differences exist in the orientation of imidazole with respect to the heme group. trans-Complementation of proximal ligand function will allow the proximal bond in hemoproteins to be chemically substituted beyond the limits of the genetic code.

摘要

在肌红蛋白(Mb)和血红蛋白(Hb)中,血红素基团的铁原子与组氨酸F8的Nε之间的近端键被认为是血红素结合、蛋白质结构和氧结合的重要决定因素。本文描述了一种系统,其中近端配体由组氨酸侧链模拟物咪唑分子间提供。利用定点诱变将抹香鲸肌红蛋白的近端配体替换为甘氨酸(H93G)。向表达该基因的大肠杆菌中添加咪唑可恢复肌红蛋白的功能。在咪唑存在下纯化的H93G肌红蛋白与多种远端配体结合时,在光谱上与野生型肌红蛋白相似。在咪唑存在下测定的H93G肌红蛋白的晶体结构表明,一个咪唑分子在近端与血红素铁结合,反式取代了野生型肌红蛋白近端组氨酸的侧链功能。尽管H93G肌红蛋白在光谱和总体结构细节上与野生型肌红蛋白相似,但咪唑相对于血红素基团的取向存在细微差异。近端配体功能的反式互补将使血红蛋白中的近端键在遗传密码的限制之外进行化学取代。

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