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NF-Y转录激活功能的保守性与差异性

Conservation and divergence of NF-Y transcriptional activation function.

作者信息

Serra E, Zemzoumi K, di Silvio A, Mantovani R, Lardans V, Dissous C

机构信息

Unité INSERM 167, Institut Pasteur Lille, 1, rue du Professeur Calmette, 59019 Lille, France.

出版信息

Nucleic Acids Res. 1998 Aug 15;26(16):3800-5. doi: 10.1093/nar/26.16.3800.

DOI:10.1093/nar/26.16.3800
PMID:9685499
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC147774/
Abstract

The CCAAT-binding protein NF-Y is involved in the regulation of a variety of eukaryotic genes and is formed in higher eukaryotes by three subunits NF-YA/B/C. We have characterized NF-Y of the trematode parasite Schistosoma mansoni and studied the structure and the function of the SMNF-YA subunit. In this work, we present the cloning and sequence analysis of the B subunit of the parasite factor. SMNF-YB contains the conserved HAP-3 homology domain but the remaining part of the protein was found to be highly divergent from all other species. We demonstrated by transfections of GAL4 fusion constructs, that mouse NF-YB does not contain activation domains while the C-terminal part of SMNF-YB has transcriptional activation potential. On the other hand, the N-terminal parts of SMNF-YA and mouse NF-YA were shown to mediate transactivation; the integrity of a large 160 amino acid glutamine-rich domain of NF-YA was required for this function and an adjacent serine- and threonine-rich domain was necessary for full activity in HepG2, but redundant in other cell types. Transactivation domains identified in SMNF-YB are also rich in serine and threonine residues. Our results indicate that serine/threonine-richsequences from helminth parasites potentiate trans-cription and that such structures have diverged during evolution within the same transcription factor.

摘要

CCAAT结合蛋白NF-Y参与多种真核基因的调控,在高等真核生物中由三个亚基NF-YA/B/C组成。我们已经对曼氏血吸虫这种吸虫寄生虫的NF-Y进行了表征,并研究了SMNF-YA亚基的结构和功能。在这项工作中,我们展示了该寄生虫因子B亚基的克隆和序列分析。SMNF-YB包含保守的HAP-3同源结构域,但发现该蛋白的其余部分与所有其他物种高度不同。我们通过转染GAL4融合构建体证明,小鼠NF-YB不包含激活结构域,而SMNF-YB的C末端部分具有转录激活潜力。另一方面,SMNF-YA和小鼠NF-YA的N末端部分显示介导反式激活;NF-YA一个大的富含160个氨基酸的谷氨酰胺结构域的完整性对于此功能是必需的,而一个相邻的富含丝氨酸和苏氨酸的结构域对于在HepG2中的完全活性是必需的,但在其他细胞类型中是多余的。在SMNF-YB中鉴定出的反式激活结构域也富含丝氨酸和苏氨酸残基。我们的结果表明,来自蠕虫寄生虫的富含丝氨酸/苏氨酸的序列增强转录,并且这种结构在同一转录因子的进化过程中已经发生了分化。

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本文引用的文献

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The two activation domains of the CCAAT-binding factor CBF interact with the dTAFII110 component of the Drosophila TFIID complex.CCAAT结合因子CBF的两个激活结构域与果蝇TFIID复合物的dTAFII110成分相互作用。
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