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金黄色葡萄球菌NAD⁺依赖性DNA连接酶腺苷酸化结构域的结构

Structure of the adenylation domain of NAD(+)-dependent DNA ligase from Staphylococcus aureus.

作者信息

Han Seungil, Chang Jeanne S, Griffor Matt

机构信息

Pfizer Inc., Groton, Connecticut 06340, USA.

出版信息

Acta Crystallogr Sect F Struct Biol Cryst Commun. 2009 Nov 1;65(Pt 11):1078-82. doi: 10.1107/S1744309109036872. Epub 2009 Oct 13.

Abstract

DNA ligase catalyzes phosphodiester-bond formation between immediately adjacent 5'-phosphate and 3'-hydroxyl groups in double-stranded DNA and plays a central role in many cellular and biochemical processes, including DNA replication, repair and recombination. Bacterial NAD(+)-dependent DNA ligases have been extensively characterized as potential antibacterial targets because of their essentiality and their structural distinction from human ATP-dependent DNA ligases. The high-resolution structure of the adenylation domain of Staphylococcus aureus NAD(+)-dependent DNA ligase establishes the conserved domain architecture with other bacterial adenylation domains. Two apo crystal structures revealed that the active site possesses the preformed NAD(+)-binding pocket and the 'C2 tunnel' lined with hydrophobic residues: Leu80, Phe224, Leu287, Phe295 and Trp302. The C2 tunnel is unique to bacterial DNA ligases and the Leu80 side chain at the mouth of the tunnel points inside the tunnel and forms a narrow funnel in the S. aureus DNA ligase structure. Taken together with other DNA ligase structures, the S. aureus DNA ligase structure provides a basis for a more integrated understanding of substrate recognition and catalysis and will be also be of help in the development of small-molecule inhibitors.

摘要

DNA连接酶催化双链DNA中紧邻的5'-磷酸基团和3'-羟基之间磷酸二酯键的形成,在包括DNA复制、修复和重组在内的许多细胞和生化过程中发挥核心作用。细菌依赖NAD(+)的DNA连接酶因其不可或缺性以及与人类依赖ATP的DNA连接酶在结构上的差异,已被广泛作为潜在的抗菌靶点进行深入研究。金黄色葡萄球菌依赖NAD(+)的DNA连接酶腺苷化结构域的高分辨率结构确定了其与其他细菌腺苷化结构域保守的结构架构。两个无配体晶体结构表明,活性位点具有预先形成的NAD(+)结合口袋以及由疏水残基(亮氨酸80、苯丙氨酸224、亮氨酸287、苯丙氨酸295和色氨酸302)排列而成的“C2通道”。C2通道是细菌DNA连接酶所特有的,通道口处的亮氨酸80侧链指向通道内部,并在金黄色葡萄球菌DNA连接酶结构中形成一个狭窄的漏斗状结构。结合其他DNA连接酶结构,金黄色葡萄球菌DNA连接酶结构为更全面地理解底物识别和催化提供了基础,也将有助于小分子抑制剂的开发。

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