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脑磷酸吡哆醛激酶的晶体结构,核糖激酶超家族的一个新成员。

Crystal structure of brain pyridoxal kinase, a novel member of the ribokinase superfamily.

作者信息

Li Ming-Hui, Kwok Francis, Chang Wen-Rui, Lau Chi-Kong, Zhang Ji-Ping, Lo Samuel C L, Jiang Tao, Liang Dong-Cai

机构信息

National Laboratory of Biomacromolecules, Institute of Biophysics, Chinese Academy of Science, Beijing 100101, China.

出版信息

J Biol Chem. 2002 Nov 29;277(48):46385-90. doi: 10.1074/jbc.M208600200. Epub 2002 Sep 15.

Abstract

The three-dimensional structures of brain pyridoxal kinase and its complex with the nucleotide ATP have been elucidated in the dimeric form at 2.1 and 2.6 A, respectively. Results have shown that pyridoxal kinase, as an enzyme obeying random sequential kinetics in catalysis, does not possess a lid shape structure common to all kinases in the ribokinase superfamily. This finding has been shown to be in line with the condition that pyridoxal kinase binds substrates with variable sizes of chemical groups at position 4 of vitamin B(6) and its derivatives. In addition, the enzyme contains a 12-residue peptide loop in the active site for the prevention of premature hydrolysis of ATP. Conserved amino acid residues Asp(118) and Tyr(127) in the peptide loop could be moved to a position covering the nucleotide after its binding so that its chance to hydrolyze in the aqueous environment of the active site was reduced. With respect to the evolutionary trend of kinase enzymes, the existence of this loop in pyridoxal kinase could be classified as an independent category in the ribokinase superfamily according to the structural feature found and mechanism followed in catalysis.

摘要

脑吡哆醛激酶及其与核苷酸ATP复合物的三维结构已分别以二聚体形式在2.1埃和2.6埃分辨率下得以阐明。结果表明,吡哆醛激酶作为一种在催化过程中遵循随机顺序动力学的酶,并不具备核糖激酶超家族中所有激酶共有的帽状结构。这一发现与吡哆醛激酶在维生素B6及其衍生物的第4位结合具有不同化学基团大小的底物这一情况相符。此外,该酶在活性位点含有一个12个残基的肽环,用于防止ATP过早水解。肽环中保守的氨基酸残基天冬氨酸(Asp118)和酪氨酸(Tyr127)在ATP结合后可移动至覆盖核苷酸的位置,从而降低其在活性位点水环境中水解的几率。就激酶的进化趋势而言,根据所发现的结构特征和催化遵循的机制,吡哆醛激酶中该环的存在在核糖激酶超家族中可归为一个独立类别。

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