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纺锤菌素和偏端霉素与脱氧核糖核酸的相互作用:电二色性研究

Interaction of netropsin and distamycin with deoxyribonucleic acid: electric dichroism study.

作者信息

Dattagupta N, Hogan M, Crothers D M

出版信息

Biochemistry. 1980 Dec 23;19(26):5998-6005. doi: 10.1021/bi00567a009.

Abstract

We report dichroism and equilibrium binding studies of netropsin (Net) and distamycin A3 (Dist) binding to deoxyribonucleic acid (DNA). We show that at low degrees of binding (r) to calf thymus DNA, Net induces a considerable increase in the apparent DNA length (14 A/drug molecule bound), closely analogous to the results reported earlier for Dist. In addition, we show that chicken erythrocyte DNA shows length changes similar to those of calf thymus DNA upon distamycin binding. DNA length reaches a maximum at 1 bound drug/20-30 base pairs and then decreases to its initial value by r = 0.1. This effect is not seen for two other DNAs with nearly identical A + T base pair content and may therefore arise from the details of base sequence or base modification in eukaryotic DNA. We also show that Dist binding to calf thymus DNA at low r values is positively cooperative and shows a DNA affinity which is primarily nonionic. We demonstrate that independent of the DNA to which they are bound, the Net and Dist transition moments are inclined by 43 +/- 3 degrees from the helix axis, consistent with the idea that both drugs bind inside and parallel to the DNA small groove. From dichroism measurements, we show that the conformational change induced in calf thymus DNA by Dist does not kink or bend the helix and does not substantially alter the average inclination of the bases. Finally, we outline a statistical mechanical theory for calculation of binding isotherms when binding is coupled to a DNA structural change.

摘要

我们报告了纺锤菌素(Net)和偏端霉素A3(Dist)与脱氧核糖核酸(DNA)结合的二色性和平衡结合研究。我们发现,在与小牛胸腺DNA的低结合度(r)下,Net会使表观DNA长度显著增加(每结合一个药物分子增加14埃),这与之前报道的Dist的结果非常相似。此外,我们还表明,偏端霉素结合后,鸡红细胞DNA的长度变化与小牛胸腺DNA相似。当每20 - 30个碱基对结合1个药物分子时,DNA长度达到最大值,然后在r = 0.1时降至初始值。对于另外两种A + T碱基对含量几乎相同的DNA,未观察到这种效应,因此这种效应可能源于真核DNA碱基序列或碱基修饰的细节。我们还表明,在低r值下,Dist与小牛胸腺DNA的结合是正协同的,并且显示出主要是非离子性的DNA亲和力。我们证明,无论与哪种DNA结合,Net和Dist的跃迁矩相对于螺旋轴倾斜43±3度,这与两种药物都在DNA小沟内并与其平行结合这一观点一致。通过二色性测量,我们表明Dist在小牛胸腺DNA中诱导的构象变化不会使螺旋扭结或弯曲,也不会显著改变碱基的平均倾斜度。最后,我们概述了一种统计力学理论,用于计算结合与DNA结构变化耦合时的结合等温线。

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