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Structural recognition between a four-way DNA junction and a resolving enzyme

机译:四向DNA连接和分辨酶之间的结构识别

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Resolving enzymes bind highly selectively to four-way DNA junctions, but the mechanism of this structural specificity is poorly understood. In this study, we have explored the role of interactions between the dimeric enzyme and the helical arms of the junction, using junctions with either shortened arms, or circular permutation of arms. We find that DNA-protein contacts in the arms containing the 5' ends of the continuous strands are very important, conferring a significant level of sequence discrimination upon both the choice of conformer and the order of strand cleavage. We have exploited these properties to obtain hydroxyl radical footprinting data on endonuclease I-junction complexes that are not complicated by the presence of alternative conformers, with results that are in good agreement with the arm permutation and shortening experiments. Substitution of phosphate groups at the center of the junction reveals the importance of electrostatic interactions at the point of strand exchange in the complex. Our data show that the form of the complex between endonuclease I and a DNA junction depends on the core of the junction and on interactions with the first six base-pairs of the arms containing the 5' ends of the continuous strands. (c) 2006 Elsevier Ltd. All rights reserved.
机译:分辨酶高度选择性地结合到四向DNA连接,但这种结构特异性的机制了解甚少。在这项研究中,我们探索了二聚体酶与连接的螺旋臂之间相互作用的作用,使用具有缩短臂或圆形排列臂的连接。我们发现,在包含连续链5'末端的臂中的DNA-蛋白质接触非常重要,在构象子的选择和链切割的顺序上赋予了显着水平的序列区分。我们已经利用这些特性获得了核酸内切酶I连接复合物上的羟基自由基足迹数据,该数据并不因存在其他构象异构体而变得复杂,其结果与臂置换和缩短实验非常吻合。在连接中心磷酸基团的取代揭示了在复合物中链交换点静电相互作用的重要性。我们的数据表明,核酸内切酶I与DNA连接之间的复合物形式取决于连接的核心以及与包含连续链5'末端的臂的前六个碱基对的相互作用。 (c)2006 Elsevier Ltd.保留所有权利。

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