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核因子 I 揭示为启动子结合转录激活因子家族。

Nuclear factor I revealed as family of promoter binding transcription activators.

机构信息

Institute of Biotechnology, University of Lausanne, Lausanne, Switzerland.

出版信息

BMC Genomics. 2011 Apr 7;12:181. doi: 10.1186/1471-2164-12-181.

DOI:10.1186/1471-2164-12-181
PMID:21473784
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3082249/
Abstract

BACKGROUND

Multiplex experimental assays coupled to computational predictions are being increasingly employed for the simultaneous analysis of many specimens at the genome scale, which quickly generates very large amounts of data. However, inferring valuable biological information from the comparisons of very large genomic datasets still represents an enormous challenge.

RESULTS

As a study model, we chose the NFI/CTF family of mammalian transcription factors and we compared the results obtained from a genome-wide study of its binding sites with chromatin structure assays, gene expression microarray data, and in silico binding site predictions. We found that NFI/CTF family members preferentially bind their DNA target sites when they are located around transcription start sites when compared to control datasets generated from the random subsampling of the complete set of NFI binding sites. NFI proteins preferably associate with the upstream regions of genes that are highly expressed and that are enriched in active chromatin modifications such as H3K4me3 and H3K36me3. We postulate that this is a causal association and that NFI proteins mainly act as activators of transcription. This was documented for one member of the family (NFI-C), which revealed as a more potent gene activator than repressor in global gene expression analysis. Interestingly, we also discovered the association of NFI with the tri-methylation of lysine 9 of histone H3, a chromatin marker previously associated with the protection against silencing of telomeric genes by NFI.

CONCLUSION

Taken together, we illustrate approaches that can be taken to analyze large genomic data, and provide evidence that NFI family members may act in conjunction with specific chromatin modifications to activate gene expression.

摘要

背景

多重实验分析与计算预测相结合,正在被越来越多地应用于在基因组范围内同时分析许多样本,这迅速产生了大量的数据。然而,从非常大的基因组数据集的比较中推断有价值的生物学信息仍然是一个巨大的挑战。

结果

作为研究模型,我们选择了哺乳动物转录因子的 NFI/CTF 家族,并将其结合位点的全基因组研究结果与染色质结构分析、基因表达微阵列数据和计算结合位点预测进行了比较。我们发现,与从 NFI 结合位点的完整集合的随机抽样生成的对照数据集相比,当 NFI/CTF 家族成员位于转录起始位点附近时,它们优先结合其 DNA 靶位点。NFI 蛋白更倾向于与高度表达的基因的上游区域结合,这些基因富含活跃的染色质修饰,如 H3K4me3 和 H3K36me3。我们推测这是一种因果关系,NFI 蛋白主要作为转录激活剂发挥作用。这在家族的一个成员(NFI-C)中得到了证明,该成员在全局基因表达分析中被证明是比抑制剂更有效的基因激活剂。有趣的是,我们还发现 NFI 与组蛋白 H3 赖氨酸 9 的三甲基化有关,这是一个先前与 NFI 保护端粒基因免受沉默相关的染色质标记。

结论

综上所述,我们说明了可以用于分析大型基因组数据的方法,并提供了证据表明 NFI 家族成员可能与特定的染色质修饰一起作用以激活基因表达。

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