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ADP - 2Ho作为含核苷酸蛋白质的相位测定工具。

ADP-2Ho as a phasing tool for nucleotide-containing proteins.

作者信息

Ku Shao-Yang, Smith G David, Howell P Lynne

机构信息

Program in Molecular Structure and Function, Research Institute, Hospital for Sick Children, 555 University Avenue, Toronto, Ontario M5G 1X8, Canada.

出版信息

Acta Crystallogr D Biol Crystallogr. 2007 Apr;63(Pt 4):493-9. doi: 10.1107/S0907444907006592. Epub 2007 Mar 16.

Abstract

Trivalent holmium ions were shown to isomorphously replace magnesium ions to form an ADP-2Ho complex in the nucleotide-binding domain of Bacillus subtilis 5-methylthioribose (MTR) kinase. This nucleotide-holmium complex provided sufficient phasing power to allow SAD and SIRAS phasing of this previously unknown structure using the L(III) absorption edge of holmium. The structure of ADP-2Ho reveals that the two Ho ions are approximately 4 A apart and are likely to share their ligands: the phosphoryl O atoms of ADP and a water molecule. The structure determination of MTR kinase using data collected using Cu Kalpha X-radiation was also attempted. Although the heavy-atom substructure determination was successful, interpretation of the map was more challenging. The isomorphous substitution of holmium for magnesium in the MTR kinase-nucleotide complex suggests that this could be a useful phasing tool for other metal-dependent nucleotide-containing proteins.

摘要

研究表明,三价钬离子可同晶取代镁离子,在枯草芽孢杆菌5-甲基硫代核糖(MTR)激酶的核苷酸结合结构域中形成ADP-2Ho复合物。这种核苷酸-钬复合物提供了足够的相位信息,能够利用钬的L(III)吸收边,对这个此前未知的结构进行单波长反常散射(SAD)和多波长反常散射(SIRAS)相位分析。ADP-2Ho的结构显示,两个钬离子相距约4埃,并且可能共享它们的配体:ADP的磷酰氧原子和一个水分子。研究人员还尝试利用铜Kα X射线收集的数据来确定MTR激酶的结构。虽然重原子子结构的确定是成功的,但图谱的解读更具挑战性。MTR激酶-核苷酸复合物中钬对镁的同晶取代表明,这可能是一种用于其他金属依赖性含核苷酸蛋白质的有用相位分析工具。

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