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p300与多个NF-Y三聚体之间的相互作用调控细胞周期蛋白B2启动子功能。

Interactions between p300 and multiple NF-Y trimers govern cyclin B2 promoter function.

作者信息

Salsi Valentina, Caretti Giuseppina, Wasner Mark, Reinhard Wibke, Haugwitz Ulrike, Engeland Kurt, Mantovani Roberto

机构信息

Dipartimento di Biologia Animale, Università di Modena e Reggio, Via Campi 213/d, 41100 Modena, Italy.

出版信息

J Biol Chem. 2003 Feb 28;278(9):6642-50. doi: 10.1074/jbc.M210065200. Epub 2002 Dec 12.

Abstract

The CCAAT box is one of the most common elements in eukaryotic promoters and is activated by NF-Y, a conserved trimeric transcription factor with histone-like subunits. Usually one CCAAT element is present in promoters at positions between -60 and -100, but an emerging class of promoters harbor multiple NF-Y sites. In the triple CCAAT-containing cyclin B2 cell-cycle promoter, all CCAAT boxes, independently from their NF-Y affinities, are important for function. We investigated the relationships between NF-Y and p300. Chromatin immunoprecipitation analysis found that NF-Y and p300 are bound to the cyclin B2 promoter in vivo and that their binding is regulated during the cell cycle, positively correlating with promoter function. Cotransfection experiments determined that the coactivator acts on all CCAAT boxes and requires a precise spacing between the three elements. We established the order of in vitro binding of the three NF-Y complexes and find decreasing affinities from the most distal Y1 to the proximal Y3 site. Binding of two or three NF-Y trimers with or without p300 is not cooperative, but association with the Y1 and Y2 sites is extremely stable. p300 favors the binding of NF-Y to the weak Y3 proximal site, provided that a correct distance between the three CCAAT is respected. Our data indicate that the precise spacing of multiple CCAAT boxes is crucial for coactivator function. Transient association to a weak site might be a point of regulation during the cell cycle and a general theme of multiple CCAAT box promoters.

摘要

CCAAT框是真核生物启动子中最常见的元件之一,可被NF-Y激活,NF-Y是一种具有组蛋白样亚基的保守三聚体转录因子。通常在启动子中,一个CCAAT元件存在于-60至-100之间的位置,但一类新兴的启动子含有多个NF-Y位点。在含有三个CCAAT的细胞周期蛋白B2细胞周期启动子中,所有CCAAT框,无论其与NF-Y的亲和力如何,对功能都很重要。我们研究了NF-Y与p300之间的关系。染色质免疫沉淀分析发现,NF-Y和p300在体内与细胞周期蛋白B2启动子结合,并且它们的结合在细胞周期中受到调节,与启动子功能呈正相关。共转染实验确定,共激活因子作用于所有CCAAT框,并且需要三个元件之间有精确的间距。我们确定了三种NF-Y复合物的体外结合顺序,发现从最远端的Y1到近端的Y3位点亲和力逐渐降低。两个或三个NF-Y三聚体与p300结合或不结合都不具有协同作用,但与Y1和Y2位点的结合极其稳定。只要三个CCAAT之间的距离正确,p300有利于NF-Y与较弱的近端Y3位点结合。我们的数据表明,多个CCAAT框的精确间距对于共激活因子功能至关重要。与弱位点的短暂结合可能是细胞周期中的一个调节点,也是多个CCAAT框启动子的一个普遍特征。

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