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一种bZip寡肽模型与模拟DNA结合位点的寡脱氧核糖核苷酸之间的相互作用。侧翼序列的影响。

Interaction of a bZip oligopeptide model with oligodeoxyribonucleotides modelling DNA binding sites. The effect of flanking sequences.

作者信息

Votavová H, Hodanová K, Arnold L, Sponar J

机构信息

Institute of Organic Chemistry and Biochemistry, Academy of Sciences of the Czech Republic, Praha, Czech Republic.

出版信息

J Biomol Struct Dyn. 1997 Dec;15(3):587-96. doi: 10.1080/07391102.1997.10508968.

Abstract

A leucine zipper (bZip) binding peptide BP1 was constructed based on the DNA binding sequence of the GCN4 protein, slightly modified to make it more similar to the sequence of other bZip proteins (Jun) with related DNA binding specificity. Self-complementary DNA hexadecanucleotides containing ATF/CRE, AP-1 and C/EPB target sites were used to study peptide-DNA complex formation. Conformation changes in both components that occur on complex formation were studied by circular dichroism (CD) spectroscopy. The results show that the amount of alpha-helix formed in the peptide strongly depends not only on the target site present, but also on the type of the sequence flanking the ATF/CRE target site. Highest amount of the alpha-helix induced in the peptide was observed when homopurine homopyrimidine flanking sequences were present, whereas the presence of alternating sequences, especially of the CA/TG type, showed considerably lower effects. The change in DNA conformation on complex formation was generally small, but also depended on the type of the flanking sequence. It appears that the sequences flanking the target site can considerably modify the ability of the target sequence to bind specifically the bZip peptide, probably by slightly varying the overall DNA conformation.

摘要

基于GCN4蛋白的DNA结合序列构建了亮氨酸拉链(bZip)结合肽BP1,并对其进行了轻微修饰,使其更类似于具有相关DNA结合特异性的其他bZip蛋白(Jun)的序列。使用含有ATF/CRE、AP-1和C/EPB靶位点的自互补DNA十六核苷酸来研究肽-DNA复合物的形成。通过圆二色性(CD)光谱研究了复合物形成时两个组分的构象变化。结果表明,肽中形成的α-螺旋量不仅强烈取决于存在的靶位点,还取决于ATF/CRE靶位点侧翼序列的类型。当存在同型嘌呤同型嘧啶侧翼序列时,观察到肽中诱导的α-螺旋量最高,而交替序列的存在,尤其是CA/TG类型,显示出相当低的影响。复合物形成时DNA构象的变化通常较小,但也取决于侧翼序列的类型。似乎靶位点侧翼的序列可以显著改变靶序列特异性结合bZip肽的能力,可能是通过稍微改变整体DNA构象来实现的。

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