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人腺嘌呤核苷酸激酶 7 和 8 的特性研究表明,腺嘌呤核苷酸激酶同工酶家族的动力学参数和结构组织存在差异。

The characterization of human adenylate kinases 7 and 8 demonstrates differences in kinetic parameters and structural organization among the family of adenylate kinase isoenzymes.

机构信息

Department of Laboratory Medicine, Karolinska Institute, Huddinge, Sweden.

出版信息

Biochem J. 2011 Feb 1;433(3):527-34. doi: 10.1042/BJ20101443.

DOI:10.1042/BJ20101443
PMID:21080915
Abstract

Differences in expression profiles, substrate specificities, kinetic properties and subcellular localization among the AK (adenylate kinase) isoenzymes have been shown to be important for maintaining a proper adenine nucleotide composition for many different cell functions. In the present study, human AK7 was characterized and its substrate specificity, kinetic properties and subcellular localization determined. In addition, a novel member of the human AK family, with two functional domains, was identified and characterized and assigned the name AK8. AK8 is the second known human AK with two complete and active AK domains within its polypeptide chain, a feature that has previously been shown for AK5. The full-length AK8, as well as its two domains AK8p1 and AK8p2, all showed similar AK enzyme activity. AK7, full-length AK8, AK8p1 and AK8p2 phosphorylated AMP, CMP, dAMP and dCMP with ATP as the phosphate donor, and also AMP, CMP and dCMP with GTP as the phosphate donor. Both AK7 and full-length AK8 showed highest affinity for AMP with ATP as the phosphate donor, and proved to be more efficient in AMP phosphorylation as compared with the major cytosolic isoform AK1. Expression of the proteins fused with green fluorescent protein demonstrated a cytosolic localization for both AK7 and AK8.

摘要

在许多不同的细胞功能中,AK(腺苷激酶)同工酶的表达谱、底物特异性、动力学特性和亚细胞定位的差异被证明对维持适当的腺嘌呤核苷酸组成很重要。在本研究中,对人 AK7 进行了表征,并确定了其底物特异性、动力学特性和亚细胞定位。此外,还鉴定和表征了人 AK 家族的一个新成员,该成员具有两个功能域,并将其命名为 AK8。AK8 是第二个已知的具有两条完整且活性 AK 结构域的人 AK,这一特征以前在 AK5 中已有报道。全长 AK8 及其两个结构域 AK8p1 和 AK8p2 均表现出相似的 AK 酶活性。AK7、全长 AK8、AK8p1 和 AK8p2 均以 ATP 为磷酸供体磷酸化 AMP、CMP、dAMP 和 dCMP,也以 GTP 为磷酸供体磷酸化 AMP、CMP 和 dCMP。AK7 和全长 AK8 均以 ATP 为磷酸供体时对 AMP 表现出最高亲和力,与主要的细胞质同工酶 AK1 相比,证明在 AMP 磷酸化方面更有效。与绿色荧光蛋白融合表达的蛋白质显示 AK7 和 AK8 均定位于细胞质。

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