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核因子Y(NF-Y)组织γ-珠蛋白CCAAT框区域。

NF-Y organizes the gamma-globin CCAAT boxes region.

作者信息

Liberati C, Ronchi A, Lievens P, Ottolenghi S, Mantovani R

机构信息

Dipartimento di Genetica e di Biologia dei Microrganismi, Università di Milano, Via Celoria 26, 20133 Milano, Italy.

出版信息

J Biol Chem. 1998 Jul 3;273(27):16880-9. doi: 10.1074/jbc.273.27.16880.

DOI:10.1074/jbc.273.27.16880
PMID:9642249
Abstract

The CCAAT-binding activator NF-Y is formed by three evolutionary conserved subunits, two of which contain putative histone-like domains. We investigated NF-Y binding to all CCAAT boxes of globin promoters in direct binding, competition, and supershift electrophoretic mobility shift assay; we found that the alpha, zeta, and proximal gamma CCAAT boxes of human and the prosimian Galago bind avidly, and distal gamma CCAAT boxes have intermediate affinity, whereas the epsilon and beta sequences bind NF-Y very poorly. We developed an efficient in vitro transcription system from erythroid K562 cells and established that both the distal and the proximal CCAAT boxes are important for optimal gamma-globin promoter activity. Surprisingly, NF-Y binding to a mutated distal CCAAT box (a C to T at position -114) is remarkably increased upon occupancy of the high affinity proximal element, located 27 base pairs away. Shortening the distance between the two CCAAT boxes progressively prevents simultaneous CCAAT binding, indicating that NF-Y interacts in a mutually exclusive way with CCAAT boxes closer than 24 base pairs apart. A combination of circular permutation and phasing analysis proved that (i) NF-Y-induced angles of the two gamma-globin CCAAT boxes have similar amplitudes; (ii) occupancy of the two CCAAT boxes leads to compensatory distortions; (iii) the two NF-Y bends are spatially oriented with combined twisting angles of about 100 degrees. Interestingly, such distortions are reminiscent of core histone-DNA interactions. We conclude that NF-Y binding imposes a high level of functionally important coordinate organization to the gamma-globin promoter.

摘要

CCAAT结合激活因子NF-Y由三个进化保守的亚基组成,其中两个含有假定的组蛋白样结构域。我们通过直接结合、竞争和超迁移电泳迁移率变动分析研究了NF-Y与珠蛋白启动子所有CCAAT框的结合;我们发现人类和原猴类夜猴的α、ζ和近端γ CCAAT框能紧密结合,而远端γ CCAAT框具有中等亲和力,而ε和β序列与NF-Y的结合非常弱。我们从红系K562细胞开发了一种高效的体外转录系统,并确定远端和近端CCAAT框对于最佳γ珠蛋白启动子活性都很重要。令人惊讶的是,当位于27个碱基对之外的高亲和力近端元件被占据时,NF-Y与突变的远端CCAAT框(-114位的C突变为T)的结合显著增加。缩短两个CCAAT框之间的距离会逐渐阻止同时结合CCAAT,这表明NF-Y以互斥的方式与距离小于24个碱基对的CCAAT框相互作用。圆形排列和相位分析相结合证明:(i)NF-Y诱导的两个γ珠蛋白CCAAT框的角度具有相似的幅度;(ii)两个CCAAT框的占据会导致补偿性扭曲;(iii)两个NF-Y弯曲在空间上的定向组合扭转角度约为100度。有趣的是,这种扭曲让人联想到核心组蛋白与DNA的相互作用。我们得出结论,NF-Y的结合为γ珠蛋白启动子赋予了高水平的功能重要的协同组织。

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