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Analysis of the eukaryotic topoisomerase II DNA gate: a single-molecule FRET and structural perspective

机译:真核生物拓扑异构酶II DNA门的分析:单分子FRET和结构的角度。

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摘要

Type II DNA topoisomerases (topos) are essential and ubiquitous enzymes that perform important intracellular roles in chromosome condensation and segregation, and in regulating DNA supercoiling. Eukaryotic topo II, a type II topoisomerase, is a homodimeric enzyme that solves topological entanglement problems by using the energy from ATP hydrolysis to pass one segment of DNA through another by way of a reversible, enzyme-bridged double-stranded break. This DNA break is linked to the protein by a phosphodiester bond between the active site tyrosine of each subunit and backbone phosphate of DNA. The opening and closing of the DNA gate, a critical step for strand passage during the catalytic cycle, is coupled to this enzymatic cleavage/religation of the backbone. This reversible DNA cleavage reaction is the target of a number of anticancer drugs, which can elicit DNA damage by affecting the cleavage/religation equilibrium. Because of its clinical importance, many studies have sought to determine the manner in which topo II interacts with DNA. Here we highlight recent single-molecule fluorescence resonance energy transfer and crystallographic studies that have provided new insight into the dynamics and structure of the topo II DNA gate.
机译:II型DNA拓扑异构酶(topos)是必不可少的普遍存在的酶,它们在染色体浓缩和分离以及调节DNA超螺旋中起重要的细胞内作用。真核拓扑II,是II型拓扑异构酶,是一种同二聚酶,它通过利用ATP水解产生的能量通过可逆的酶桥双链断裂,使一个DNA片段通过另一个片段,从而解决了拓扑纠缠问题。该DNA断裂通过每个亚基的活性位点酪氨酸与DNA的主链磷酸之间的磷酸二酯键与蛋白质连接。 DNA门的打开和关闭是催化循环过程中链通过的关键步骤,与骨架的这种酶促裂解/重新连接有关。这种可逆的DNA裂解反应是许多抗癌药物的目标,它们可以通过影响裂解/连接平衡来引发DNA损伤。由于其临床重要性,许多研究试图确定topo II与DNA相互作用的方式。在这里,我们重点介绍了最近的单分子荧光共振能量转移和晶体学研究,这些研究为topo II DNA门的动力学和结构提供了新的见识。

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