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Direct regulation of topoisomerase activity by a nucleoid-associated protein

机译:核苷酸相关蛋白直接调节拓扑异构酶活性

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The topological homeostasis of bacterial chromosomes is maintained by the balance between compaction and the topological organization of genomes. Two classes of proteins play major roles in chromosome organization: the nucleoid-associated proteins (NAPs) and topoisomerases. The NAPs bind DNA to compact the chromosome, whereas topoisomerases catalytically remove or introduce supercoils into the genome. We demonstrate that HU, a major NAP of Mycobacterium tuberculosis specifically stimulates the DNA relaxation ability of mycobacterial topoisomerase I (TopoI) at lower concentrations but interferes at higher concentrations. A direct physical interaction between M. tuberculosis HU (MtHU) and TopoI is necessary for enhancing enzyme activity both in vitro and in vivo. The interaction is between the amino terminal domain of MtHU and the carboxyl terminal domain of TopoI. Binding of MtHU did not affect the two catalytic trans-esterification steps but enhanced the DNA strand passage, requisite for the completion of DNA relaxation, a new mechanism for the regulation of topoisomerase activity. An interaction-deficient mutant of MtHU was compromised in enhancing the strand passage activity. The species-specific physical and functional cooperation between MtHU and TopoI may be the key to achieve the DNA relaxation levels needed to maintain the optimal superhelical density of mycobacterial genomes.
机译:细菌染色体的拓扑动态平衡是通过紧缩和基因组拓扑结构之间的平衡来维持的。两类蛋白质在染色体组织中起主要作用:核苷相关蛋白质(NAP)和拓扑异构酶。 NAP结合DNA来压缩染色体,而拓扑异构酶则催化去除超螺旋或将超螺旋引入基因组。我们证明,HU,结核分枝杆菌的主要NAP会在较低浓度下特异性刺激分支杆菌拓扑异构酶I(TopoI)的DNA松弛能力,但在较高浓度下会产生干扰。结核分枝杆菌HU(MtHU)和TopoI之间的直接物理相互作用对于增强体内和体外酶的活性是必要的。相互作用是在MtHU的氨基末端结构域和TopoI的羧基末端结构域之间。 MtHU的结合不会影响两个催化的酯交换步骤,但会增加DNA链的通过,这是完成DNA松弛(调节拓扑异构酶活性的新机制)所必需的。 MtHU的缺乏相互作用的突变体在增强链通过活性中受到损害。 MtHU和TopoI之间物种特异性的物理和功能合作可能是达到维持分枝杆菌基因组最佳超螺旋密度所需的DNA松弛水平的关键。

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    《Nucleic Acids Research》 |2014年第17期|共10页
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