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通过环化分析测定富含G/C序列的弯曲和扭转灵活性。

Bending and torsional flexibility of G/C-rich sequences as determined by cyclization assays.

作者信息

Dlakic M, Harrington R E

机构信息

Department of Biochemistry, University of Nevada, Reno 89557-0014, USA.

出版信息

J Biol Chem. 1995 Dec 15;270(50):29945-52. doi: 10.1074/jbc.270.50.29945.

DOI:10.1074/jbc.270.50.29945
PMID:8530394
Abstract

The structural polymorphism of DNA is a vital aspect of its biological function. However, it has become increasingly apparent in recent years that DNA polymorphism is a complicated, multidimensional phenomenon that includes not only static sequence-directed structures but dynamic effects as well, including influences of counterions and sequence context. In order to address some of these additional factors that govern DNA conformation, we have used T4 ligase-mediated cyclization to investigate bending in a series of DNA sequences containing the GGGCCC.GGGCCC motif in different sequence contexts including various helical phasings with (A)5-tracts. We present evidence for curvature in GGGCCC.GGGCCC and (A)5-tract motifs in the presence of physiological levels of Mg2+ and show that these motifs curve through similar but oppositely directed bending angles under these ionic strength conditions. Although these two sequence motifs appear to bend similarly, our results suggest significant differences in stiffness and stability of curvature between them. We also show that under the same experimental conditions, the CTAG-CTAG sequence element possesses unusual torsional flexibility and that this appears to be associated with the central TA.TA dinucleotide. The results underscore the need to include sequence context and specific ion effects as well as a dynamic basis in more complete predictive models for functionally related DNA polymorphism.

摘要

DNA的结构多态性是其生物学功能的一个重要方面。然而,近年来越来越明显的是,DNA多态性是一种复杂的、多维度的现象,它不仅包括静态的序列导向结构,还包括动态效应,包括抗衡离子和序列环境的影响。为了研究一些控制DNA构象的其他因素,我们利用T4连接酶介导的环化反应,研究了一系列在不同序列环境中包含GGGCCC.GGGCCC基序的DNA序列的弯曲情况,这些序列环境包括与(A)5-序列段的各种螺旋相位。我们提供了在生理水平的Mg2+存在下GGGCCC.GGGCCC和(A)5-序列段基序中存在曲率的证据,并表明在这些离子强度条件下,这些基序通过相似但方向相反的弯曲角度弯曲。尽管这两个序列基序似乎弯曲方式相似,但我们的结果表明它们在曲率的刚度和稳定性方面存在显著差异。我们还表明,在相同的实验条件下,CTAG-CTAG序列元件具有不寻常的扭转灵活性,这似乎与中心TA.TA二核苷酸有关。这些结果强调,在更完整的功能相关DNA多态性预测模型中,需要纳入序列环境、特定离子效应以及动态基础。

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Bending and torsional flexibility of G/C-rich sequences as determined by cyclization assays.通过环化分析测定富含G/C序列的弯曲和扭转灵活性。
J Biol Chem. 1995 Dec 15;270(50):29945-52. doi: 10.1074/jbc.270.50.29945.
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