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Rotation of DNA around intact strand in human topoisomerase I implies distinct mechanisms for positive and negative supercoil relaxation

机译:DNA在人类拓扑异构酶I完整链周围的旋转暗示了正负超螺旋松弛的独特机制

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Topoisomerases are enzymes of quintessence to the upkeep of superhelical DNA, and are vital for replication, transcription and recombination. An atomic-resolution model for human topoisomerase I in covalent complex with DNA is simulated using molecular dynamics with external potentials that mimic torque and bias the DNA duplex downstream of a single-strand cut to rotate around the intact strand, according to the prevailing enzymatic mechanism. The simulations reveal the first dynamical picture of how topoisomerase accommodates large-scale motion of DNA as it changes its supercoiling state, and indicate that relaxation of positive and negative supercoils are fundamentally different. To relax positive supercoils, two separate domains (the ‘lips') of the protein open up by about 10–14 ?, whereas to relax negative supercoils, a continuous loop connecting the upper and lower parts (and which was a hinge for opening the lips) stretches about 12 ? while the lips remain unseparated. Normal mode analysis is additionally used to characterize the functional flexibility of the protein. Remarkably, the same combination of low-frequency eigenvectors exhibit the dominant contribution for both rotation mechanisms through a see-saw motion. The simulated mechanisms suggest mutations to control the relaxation of either type of supercoiling selectively and advance a hypothesis for the debated role of the N-terminal domain in supercoil relaxation.
机译:拓扑异构酶是精通超螺旋DNA维持的典型酶,对于复制,转录和重组至关重要。根据流行的酶促机理,使用具有外部电势的分子动力学模拟了人类拓扑异构酶I与DNA共价复合物的原子分辨率模型,该分子动力学模仿了扭矩并使单链切割下游的DNA双链体偏向于围绕完整链旋转, 。模拟揭示了拓扑异构酶如何适应DNA改变其超螺旋状态时的大规模运动的第一动力学图,并表明正负超级螺旋的弛豫本质上不同。要放松正性超螺旋,蛋白质的两个独立结构域(“唇”)张开约10–14 ?,而要放松负性超螺旋,则是一个连续的环,将上部和下部连接在一起(并且这是一个打开蛋白核的铰链)。嘴唇)舒展约12?而嘴唇保持不分离。另外,使用普通模式分析来表征蛋白质的功能灵活性。值得注意的是,低频特征向量的相同组合通过跷跷板运动展现了两种旋转机制的主要作用。模拟的机制表明突变,以选择性地控制两种类型的超螺旋的弛豫,并提出了关于N末端结构域在超螺旋弛豫中争论作用的假设。

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