Pax-5 (BSAP) recruits Ets proto-oncogene family proteins to form functional ternary complexes on a B-cell-specific promoter

被引:205
作者
Fitzsimmons, D
Hodsdon, W
Wheat, W
Maira, SM
Wasylyk, B
Hagman, J
机构
[1] NATL JEWISH CTR IMMUNOL & RESP MED,DIV BASIC IMMUNOL,DENVER,CO 80206
[2] UNIV COLORADO,HLTH SCI CTR,DEPT IMMUNOL,DENVER,CO 80262
[3] INST GENET & BIOL MOL & CELLULAIRE,ILLKIRCH GRAFFENS,FRANCE
关键词
B-cell-specific ternary complex; Net; elk-1; SAP1a; mb-1; promoter;
D O I
10.1101/gad.10.17.2198
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
The paired box transcription factor Pax-5 (B-cell-specific activator protein) is a key regulator of lineage-specific gene expression and differentiation in B-lymphocytes. We show that Pax-5 functions as a cell type-specific docking protein that facilitates binding of the early B-cell-specific mb-1 promoter by proteins of the Ets proto-oncogene family. Transcriptional activity of the mb-1 promoter in pre-B-cells is critically dependent on binding sites for Pax-5:Ets complexes. Ternary complex assembly requires only the Pas-5 paired box and ETS DNA-binding domains. Mutation of a single base pair in the ternary complex binding site allows for independent binding by Ets proteins but, conversely, inhibits the binding of Pax-5 by itself. Strikingly, the mutation reverses the pattern of complex assembly: Ets proteins recruit Pax-5 to bind the mutated sequence. Recruitment of Net acid Elk-1, but not SAP1a, by Pax-5 defines a functional difference between closely related Ets proteins. Replacement of a valine (V68) in the ETS domain of SAP1a by aspartic acid (as found in c-Ets-1, Elk-1, and Net) enhanced ternary complex formation by more than 60-fold. Together, these observations define novel transcription factor interactions that regulate gene expression in B cells.
引用
收藏
页码:2198 / 2211
页数:14
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