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Oct-1与DNA结合后发生的构象改变决定了其与相关转录共激活因子差异相互作用中的选择性。

Conformational alteration of Oct-1 upon DNA binding dictates selectivity in differential interactions with related transcriptional coactivators.

作者信息

Misra V, Walter S, Yang P, Hayes S, O'Hare P

机构信息

Saskatchewan Health Services Utilization and Research Commission, Canada.

出版信息

Mol Cell Biol. 1996 Aug;16(8):4404-13. doi: 10.1128/MCB.16.8.4404.

DOI:10.1128/MCB.16.8.4404
PMID:8754841
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC231439/
Abstract

VP16 (termed VP16-H here) of herpes simplex virus (HSV) belongs to a family of related regulatory proteins which includes VP16-B of bovine herpesvirus (BHV). We show that VP16-B, while also being a powerful transactivator of transcription dependent on Oct-1 binding sites in its target promoters, has virtually no activity on a defined VP16-H-responsive, octamer-containing target promoter. While Oct-1 binds equally well to the VP16-B-responsive and -nonresponsive sites, VP16-B interacts with Oct-1 only when Oct-1 is bound to the BHV octamer site and not when it is bound to the HSV site. We show from the analysis of chimeric proteins that the ability of VP16-B to discriminate between the Oct-1 forms depends on features of its N-terminal region. We also show from an analysis of chimeric DNA motifs that sequences that lie 3' to the POU domain-contacting region of the HSV octamer site play a role in making it unresponsive to VP16-B. Finally, we show by high-resolution hydroxyl radical footprint analysis that the conformation of Oct-l is different on the two sites. These results augment our previous report on an allosteric effect of DNA signals on the conformation of bound proteins and indicate that different conformations of the same DNA binding protein can be recognized selectively by related members of interacting regulatory proteins. The possible implications of our observations for selective gene regulation by Oct-1, a ubiquitous transcription factor, and other multimember transcription families are discussed.

摘要

单纯疱疹病毒(HSV)的VP16(此处称为VP16-H)属于一类相关的调节蛋白家族,其中包括牛疱疹病毒(BHV)的VP16-B。我们发现,VP16-B虽然也是一种依赖其靶启动子中Oct-1结合位点的强大转录反式激活因子,但对一个明确的含八聚体的VP16-H反应性靶启动子几乎没有活性。虽然Oct-1与VP16-B反应性和非反应性位点的结合能力相同,但VP16-B仅在Oct-1与BHV八聚体位点结合时与其相互作用,而在Oct-1与HSV位点结合时则不相互作用。我们通过对嵌合蛋白的分析表明,VP16-B区分Oct-1不同形式的能力取决于其N端区域的特征。我们还通过对嵌合DNA基序的分析表明,HSV八聚体位点的POU结构域接触区域3'端的序列在使其对VP16-B无反应中起作用。最后,我们通过高分辨率羟基自由基足迹分析表明,Oct-1在这两个位点上的构象不同。这些结果扩展了我们之前关于DNA信号对结合蛋白构象的变构效应的报告,并表明相互作用的调节蛋白的相关成员可以选择性地识别同一DNA结合蛋白的不同构象。我们讨论了这些观察结果对Oct-1(一种普遍存在的转录因子)和其他多成员转录家族进行选择性基因调控的可能影响。

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