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CCAAT结合因子CBF的A亚基中的三类突变描绘了参与CBF-DNA复合物三步组装的功能结构域。

Three classes of mutations in the A subunit of the CCAAT-binding factor CBF delineate functional domains involved in the three-step assembly of the CBF-DNA complex.

作者信息

Sinha S, Kim I S, Sohn K Y, de Crombrugghe B, Maity S N

机构信息

Department of Molecular Genetics, University of Texas M. D. Anderson Cancer Center, Houston 77030, USA.

出版信息

Mol Cell Biol. 1996 Jan;16(1):328-37. doi: 10.1128/MCB.16.1.328.

Abstract

The mammalian CCAAT-binding factor CBF (also called NF-Y or CP1) consists of three subunits, CBF-A, CBF-B, and CBF-C, all of which are required for DNA binding and present in the CBF-DNA complex. In this study we first established the stoichiometries of the CBF subunits, both in the CBF molecule and in the CBF-DNA complex, and showed that one molecule of each subunit is present in the complex. To begin to understand the interactions between the CBF subunits and DNA, we performed a mutational analysis of the CBF-A subunit. This analysis identified three classes of mutations in the segment of CBF-A that is conserved in Saccharomyces cerevisiae and mammals. Analysis of the first class of mutants revealed that a major part of the conserved segment was essential for interactions with CBF-C to form a heterodimeric CBF-A/CBF-C complex. The second class of mutants identified a segment of CBF-A that is necessary for interactions between the CBF-A/CBF-C heterodimer and CBF-B to form a CBF heterotrimer. The third class defined a domain of CBF-A involved in binding the CBF heterotrimer to DNA. The second and third classes of mutants acted as dominant negative mutants inhibiting the formation of a complex between the wild-type CBF subunits and DNA. The segment of CBF-A necessary for DNA binding showed sequence homology to a segment of CBF-C. Interestingly, these sequences in CBF-A and CBF-C were also homologous to the sequences in the histone-fold motifs of histones H2B and H2A, respectively, and to the archaebacterial histone-like protein HMf-2. We discuss the functional domains of CBF-A and the properties of CBF in light of these sequence homologies and propose that an ancient histone-like motif in two CBF subunits controls the formation of a heterodimer between these subunits and the assembly of a sequence-specific DNA-protein complex.

摘要

哺乳动物CCAAT结合因子CBF(也称为NF-Y或CP1)由三个亚基组成,即CBF-A、CBF-B和CBF-C,它们都是DNA结合所必需的,并且存在于CBF-DNA复合物中。在本研究中,我们首先确定了CBF亚基在CBF分子和CBF-DNA复合物中的化学计量,并表明复合物中每个亚基各有一个分子。为了开始了解CBF亚基与DNA之间的相互作用,我们对CBF-A亚基进行了突变分析。该分析在酿酒酵母和哺乳动物中保守的CBF-A片段中鉴定出三类突变。对第一类突变体的分析表明,保守片段的主要部分对于与CBF-C相互作用形成异二聚体CBF-A/CBF-C复合物至关重要。第二类突变体鉴定出一段CBF-A片段,它是CBF-A/CBF-C异二聚体与CBF-B相互作用形成CBF异三聚体所必需的。第三类突变定义了CBF-A中一个与将CBF异三聚体结合到DNA有关的结构域。第二类和第三类突变体作为显性负突变体,抑制野生型CBF亚基与DNA之间复合物的形成。与DNA结合所必需的CBF-A片段与CBF-C的一段序列具有同源性。有趣的是,CBF-A和CBF-C中的这些序列分别也与组蛋白H2B和H2A的组蛋白折叠基序中的序列同源,并且与古细菌组蛋白样蛋白HMf-2同源。我们根据这些序列同源性讨论了CBF-A的功能结构域和CBF的特性,并提出两个CBF亚基中一个古老的组蛋白样基序控制这些亚基之间异二聚体的形成以及序列特异性DNA-蛋白质复合物的组装。

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