The B cell coactivator Bob1 shows DNA sequence-dependent complex formation with Oct-1/Oct-2 factors, leading to differential promoter activation

被引:124
作者
Gstaiger, M
Georgiev, O
vanLeeuwen, H
vanderVliet, P
Schaffner, W
机构
[1] UNIV ZURICH, INST MOL BIOL 2, CH-8057 ZURICH, SWITZERLAND
[2] UNIV UTRECHT, PHYSIOL CHEM LAB, 3508 TA UTRECHT, NETHERLANDS
关键词
B-cell coactivators; DNA binding specificity; POU factors; protein-protein interaction; transcriptional activation;
D O I
10.1002/j.1460-2075.1996.tb00638.x
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
We have shown previously that both octamer binding transcription factors, namely the ubiquitous Oct-1 and the B cell-specific Oct-2A protein, can be enhanced in transcriptional activity by their association with the B cell-specific coactivator protein Bob1, also called OBF-1 or OCA-B, Here we study the structural requirements for ternary complex formation of DNA-Oct-Bob1 and coactivation function of Bob1, In analogy to DNA-bound transcription factors, Bob1 has a modular structure that includes an interaction domain (amino acids 1-65) and a C-terminal domain (amino acids 65-256), both important for transcriptional activation, A mutational analysis has resolved a region of seven amino acids (amino acids 26-32) in the N-terminus of Bob1 that are important for contacting the DNA binding POU domain of Oct-1 or Oct-2, In contrast to the viral coactivator VP16 (vmw65), which interacts with Oct-1 via the POU homeosubdomain, Bob1 association with Oct factors requires residues located in the POU-specific subdomain. Because the same residues are also involved in DNA recognition, we surmised that this association would affect the DNA binding specificity of the Oct-Bob1 complex compared with free Oct factors. While Oct-1 or Oct-2 bind to a large variety of octamer sequences, Bob1 ternary complex formation is indeed highly selective and occurs only in a subset of these sequences, leading to the differential coactivation of octamer-containing promoters. The results uncover a new level in selectivity that furthers our understanding in the regulation of cell type-specific gene expression.
引用
收藏
页码:2781 / 2790
页数:10
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