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首页> 外文期刊>Nucleic Acids Research >Tryptophane-205 of human topoisomerase I is essential for camptothecin inhibition of negative but not positive supercoil removal
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Tryptophane-205 of human topoisomerase I is essential for camptothecin inhibition of negative but not positive supercoil removal

机译:人拓扑异构酶I的色氨酸205对于喜树碱抑制超螺旋去除的负作用而不是阳性

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摘要

Positive supercoils are introduced in cellular DNA in front of and negative supercoils behind tracking polymerases. Since DNA purified from cells is normally under-wound, most studies addressing the relaxation activity of topoisomerase I have utilized negatively supercoiled plasmids. The present report compares the relaxation activity of human topoisomerase I variants on plasmids containing equal numbers of superhelical twists with opposite handedness. We demonstrate that the wild-type enzyme and mutants lacking amino acids 1206 or 191206, or having tryptophane-205 replaced with a glycine relax positive supercoils faster than negative supercoils under both processive and distributive conditions. In contrast to wild-type topoisomerase I, which exhibited camptothecin sensitivity during relaxation of both negative and positive supercoils, the investigated N-terminally mutated variants were sensitive to camptothecin only during removal of positive supercoils. These data suggest different mechanisms of action during removal of supercoils of opposite handedness and are consistent with a recently published simulation study [Sari and Andricioaei (2005) Nucleic Acids Res., 33, 66216634] suggesting flexibility in distinct parts of the enzyme during clockwise or counterclockwise strand rotation.
机译:阳性超螺旋在追踪聚合酶之前被引入细胞DNA中,而阴性超螺旋则被引入跟踪之后。由于从细胞中纯化的DNA通常在伤口上,因此大多数有关拓扑异构酶I松弛活性的研究都使用了负超螺旋质粒。本报告比较了人类拓扑异构酶I变体在质粒中含有相等数量的具有相反旋向性的超螺旋扭曲的松弛活性。我们证明了野生型酶和突变体缺乏氨基酸1206或191206,或色氨酸205被甘氨酸替代在过程性和分配性条件下比负超螺旋更快地松弛正超螺旋。与野生型拓扑异构酶I(在阴性和阳性超螺旋均松弛期间表现出喜树碱敏感性)相反,研究的N端突变变体仅在去除阳性超螺旋时才对喜树碱敏感。这些数据表明在反手性超螺旋的去除过程中有不同的作用机理,并且与最近发表的模拟研究[Sari and Andricioaei(2005)Nucleic Acids Res。,33,66216634]一致,表明顺时针或逆时针在酶的不同部分具有柔性。逆时针旋转钢绞线。

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