Literature DB >> 26028650

Transactivation Function-2 of Estrogen Receptor α Contains Transactivation Function-1-regulating Element.

Yukitomo Arao1, Laurel A Coons2, William J Zuercher3, Kenneth S Korach4.   

Abstract

ERα has a ligand-dependent transactivation function in the ligand binding domain of ERα C terminus (AF-2) and a ligand-independent activation function in the N terminus (AF-1). It is still not fully understood how AF-1 and AF-2 activities are regulated cooperatively by ligands. To evaluate the AF-1 involvement in the estrogenic activities of various compounds, we analyzed these transactivation functions using AF-1-truncated and AF-2-mutated ERα mutants. AF-2 is composed of two domains with flexible and static regions. We used an AF-2 flexible region mutant and an AF-2 static region mutant. Both mutants have been reported as non-E2 responsive due to disruption of E2-mediated coactivator recruitment to the AF-2. The AF-2 mutants were not activated by agonists, but surprisingly antagonists and selective estrogen receptor modulators (SERMs) activated the AF-2 mutants. This antagonist reversal activity was derived from AF-1. Furthermore, we demonstrated that the AF-2 contains an AF-1 suppression function using C-terminal-truncated ERα mutants. From these findings we hypothesized that the mutation of AF-2 disrupted its ability to suppress AF-1, causing the antagonist reversal. To assess the AF-2-mediated AF-1 suppression, we analyzed the transcription activity of physically separated AF-1 and AF-2 using a novel hybrid reporter assay. We observed that the AF-1 activity was not suppressed by the physically separated AF-2. Furthermore, SERMs did not induce the AF-1-mediated activity from the separated mutant AF-2, which differed from the intact protein. These results imply that SERM activity is dependent on a conformational change of the full-length ERα molecule, which allows for AF-1 activation.
© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.

Entities:  

Keywords:  agonist; antagonist; estrogen; estrogen receptor; protein structure; selected estrogen receptor modulators; steroid hormone; steroid hormone receptor

Mesh:

Substances:

Year:  2015        PMID: 26028650      PMCID: PMC4498094          DOI: 10.1074/jbc.M115.638650

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  28 in total

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4.  Long-Term Follow-Up and Treatment of a Female With Complete Estrogen Insensitivity.

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7.  The genomic regulatory elements for estrogen receptor alpha transactivation-function-1 regulated genes.

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10.  Hormone signaling and fatty liver in females: analysis of estrogen receptor α mutant mice.

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