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多胺会改变序列特异性的DNA-蛋白质相互作用。

Polyamines alter sequence-specific DNA-protein interactions.

作者信息

Panagiotidis C A, Artandi S, Calame K, Silverstein S J

机构信息

Department of Microbiology, College of Physicians and Surgeons, Columbia University, New York, NY 10032, USA.

出版信息

Nucleic Acids Res. 1995 May 25;23(10):1800-9. doi: 10.1093/nar/23.10.1800.

Abstract

The polyamines are abundant biogenic cations implicated in many biological processes. Despite a plethora of evidence on polyamine-induced DNA conformational changes, no thorough study of their effects on the activities of sequence-specific DNA binding proteins has been performed. We describe the in vitro effects of polyamines on the activities of purified, representative DNA-binding proteins, and on complex protein mixtures. Polyamines at physiological concentrations enhance the binding of several proteins to DNA (e.g. USF, TFE3, Ig/EBP, NF-IL6, YY1 and ICP-4, a herpes simplex virus gene regulator), but inhibit others (e.g. Oct-1). The degree of enhancement correlates with cationic charge; divalent putrescine is ineffective whereas tetravalent spermine is more potent than trivalent spermidine. Polyamine effects on USF and ICP-4 result from increased rate of complex formation rather than a decreased rate of dissociation. DNAse I footprint analysis indicated that polyamines do not alter DNA-protein contacts. Polyamines also facilitate formation of complexes involving binding of more than one protein on a DNA fragment.

摘要

多胺是一类丰富的生物阳离子,参与许多生物学过程。尽管有大量证据表明多胺可诱导DNA构象变化,但尚未对其对序列特异性DNA结合蛋白活性的影响进行全面研究。我们描述了多胺在体外对纯化的代表性DNA结合蛋白以及复杂蛋白质混合物活性的影响。生理浓度的多胺可增强几种蛋白质与DNA的结合(例如USF、TFE3、Ig/EBP、NF-IL6、YY1和单纯疱疹病毒基因调节因子ICP-4),但会抑制其他蛋白质(例如Oct-1)。增强程度与阳离子电荷相关;二价腐胺无效,而四价精胺比三价亚精胺更有效。多胺对USF和ICP-4的影响源于复合物形成速率的增加,而非解离速率的降低。DNA酶I足迹分析表明,多胺不会改变DNA-蛋白质接触。多胺还促进了涉及一种以上蛋白质结合到DNA片段上的复合物的形成。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bfd2/306939/69d90107b88f/nar00010-0166-a.jpg

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