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两种嗜盐核苷二磷酸激酶不同盐依赖性酶活性的分子机制

Molecular mechanism of distinct salt-dependent enzyme activity of two halophilic nucleoside diphosphate kinases.

作者信息

Yamamura Akihiro, Ichimura Takefumi, Kamekura Masahiro, Mizuki Toru, Usami Ron, Makino Tsukasa, Ohtsuka Jun, Miyazono Ken-ichi, Okai Masahiko, Nagata Koji, Tanokura Masaru

机构信息

Department of Applied Biological Chemistry, Graduate School of Agricultural and Life Sciences, University of Tokyo, Bunkyo-ku, Tokyo 113-8657, Japan.

出版信息

Biophys J. 2009 Jun 3;96(11):4692-700. doi: 10.1016/j.bpj.2009.03.012.

DOI:10.1016/j.bpj.2009.03.012
PMID:19486691
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2711501/
Abstract

Nucleoside diphosphate kinases from haloarchaea Haloarcula quadrata (NDK-q) and H. sinaiiensis (NDK-s) are identical except for one out of 154 residues, i.e., Arg(31) in NDK-q and Cys(31) in NDK-s. However, the salt-dependent activity profiles of NDK-q and NDK-s are quite different: the optimal NaCl concentrations of NDK-q and NDK-s are 1 M and 2 M, respectively. We analyzed the relationships of the secondary, tertiary, and quaternary structures and NDK activity of these NDKs at various salt concentrations, and revealed that 1), NDK-q is present as a hexamer under a wide range of salt concentrations (0.2-4 M NaCl), whereas NDK-s is present as a hexamer at an NaCl concentration above 2 M and as a dimer at NaCl concentrations below 1 M; 2), dimeric NDK-s has lower activity than hexameric NDK-s; and 3), dimeric NDK-s has higher helicity than hexameric NDK-s. We also determined the crystal structure of hexameric NDK-q, and revealed that Arg(31) plays an important role in stabilizing the hexamer. Thus the substitution of Arg (as in NDK-q) to Cys (as in NDK-s) at position 31 destabilizes the hexameric assembly, and causes dissociation to less active dimers at low salt concentrations.

摘要

来自嗜盐古菌四方形嗜盐嗜碱菌(NDK-q)和中华嗜盐嗜碱菌(NDK-s)的核苷二磷酸激酶,除了154个残基中的一个不同外完全相同,即NDK-q中的精氨酸(31)和NDK-s中的半胱氨酸(31)。然而,NDK-q和NDK-s的盐依赖性活性曲线却大不相同:NDK-q和NDK-s的最佳氯化钠浓度分别为1 M和2 M。我们分析了这些核苷二磷酸激酶在不同盐浓度下的二级、三级和四级结构与活性之间的关系,结果表明:1)NDK-q在很宽的盐浓度范围(0.2 - 4 M氯化钠)下以六聚体形式存在,而NDK-s在氯化钠浓度高于2 M时以六聚体形式存在,在氯化钠浓度低于1 M时以二聚体形式存在;2)二聚体形式的NDK-s活性低于六聚体形式的NDK-s;3)二聚体形式的NDK-s比六聚体形式的NDK-s具有更高的螺旋度。我们还测定了六聚体NDK-q的晶体结构,结果表明精氨酸(31)在稳定六聚体中起重要作用。因此,在第31位将精氨酸(如在NDK-q中)替换为半胱氨酸(如在NDK-s中)会使六聚体组装不稳定,并导致在低盐浓度下解离为活性较低的二聚体。