期刊
JOURNAL OF BIOLOGICAL CHEMISTRY
卷 276, 期 26, 页码 23838-23848出版社
AMER SOC BIOCHEMISTRY MOLECULAR BIOLOGY INC
DOI: 10.1074/jbc.M102166200
关键词
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Triiodothyronine (T3) stimulates a robust increase (40-fold) in transcription of the malic enzyme gene in chick embryo hepatocytes. Previous work has shown that optimal T3 regulation of malic enzyme transcription is dependent on the presence of an accessory element (designated as region E) that immediately flanks a cluster of five T3 response elements in the malic enzyme gene. Here, we have analyzed the binding of nuclear proteins to region E and investigated the mechanism by which region E enhances T3 responsiveness. In nuclear extracts hom hepatocytes, region E binds heterodimeric complexes consisting of the homeodomain proteins PBX and MEIS1, Region E contains four consecutive PBX/MEIS1 half-sites, PBX-MEIS1 heterodimers bind the first and second half-sites, the third and fourth half-sites, and the first and fourth half-sites. The configuration conferring the greatest increase in T3 responsiveness consists of the first and fourth half-sites that are separated by 7 nucleotides. Stimulation of T3 response element functions by region E does not require the presence of additional melic enzyme sequences. In pull-down experiments, PBX1a and PBX1b specifically bind the nuclear T3 receptor-or, and this interaction is enhanced by the presence of T3, A T3 receptor-ct region containing the DNA binding domain plus nanking sequences famine acids 21-157) is necessary and sufficient for binding to PBX1a and PBX1b, These results indicate that PBX-MEIS1 complexes interact with nuclear T3 receptors to enhance T3 regulation of malic enzyme transcription in hepatocytes.
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