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Complexity in the binding of minor groove agents: netropsin has two thermodynamically different DNA binding modes at a single site

机译:小沟剂结合的复杂性:netropsin在单个位点具有两种热力学不同的DNA结合模式

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摘要

Structural results with minor groove binding agents, such as netropsin, have provided detailed, atomic level views of DNA molecular recognition. Solution studies, however, indicate that there is complexity in the binding of minor groove agents to a single site. Netropsin, for example, has two DNA binding enthalpies in isothermal titration calorimetry (ITC) experiments that indicate the compound simultaneously forms two thermodynamically different complexes at a single AATT site. Two proposals for the origin of this unusual observation have been developed: (i) two different bound species of netropsin at single binding sites and (ii) a netropsin induced DNA hairpin to duplex transition. To develop a better understanding of DNA recognition complexity, the two proposals have been tested with several DNAs and the methods of mass spectrometry (MS), polyacrylamide gel electrophoresis (PAGE) and nuclear magnetic resonance spectroscopy in addition to ITC. All of the methods with all of the DNAs investigated clearly shows that netropsin forms two different complexes at AATT sites, and that the proposal for an induced hairpin to duplex transition in this system is incorrect.
机译:使用较小的沟槽结合剂(如netropsin)的结构结果提供了DNA分子识别的详细原子级视图。但是,溶液研究表明,小沟剂与单个位点的结合很复杂。例如,Netropsin在等温滴定量热(ITC)实验中具有两个DNA结合焓,表明该化合物在单个AATT位点同时形成两个热力学不同的复合物。对于这种异常观察的起源,已经提出了两个建议:(i)Netropsin在单一结合位点的两种不同结合物种,以及(ii)Netropsin诱导的DNA发夹向双链体转变。为了更好地理解DNA识别的复杂性,这两个提案已通过几种DNA进行了测试,除ITC以外,还采用了质谱(MS),聚丙烯酰胺凝胶电泳(PAGE)和核磁共振波谱方法。所有研究了所有DNA的方法均清楚地表明,netropsin在AATT位点形成两种不同的复合物,并且在该系统中诱导发夹向双链体转变的建议是错误的。

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