Literature DB >> 15193453

Corepressor recruitment by agonist-bound nuclear receptors.

John H White1, Isabelle Fernandes, Sylvie Mader, Xiang-Jiao Yang.   

Abstract

Members of the nuclear receptor superfamily are ligand-regulated transcription factors that are composed of a series of conserved domains. These receptors are targets of a wide range of lipophilic signaling molecules that modulate many aspects of physiology and metabolism. Binding of cognate ligands to receptors induces a conformational change in the ligand binding domain (LBD) that creates a pocket for recruitment of coregulatory proteins, which are essential for ligand-dependent regulation of transcription. Several coregulatory proteins that interact with hormone-bound receptors contain characteristic helical LXXLL motifs, known as nuclear receptor (NR) boxes. Generally, ligand binding to receptors is associated with activation of transcription, and most of the NR box-containing proteins characterized to date are coactivators. However, a full understanding of the function of hormone-bound receptors must also incorporate their recruitment of corepressors. The recent identification of ligand-dependent corepressor (LCoR) is a case in point. LCoR contains a single NR box that mediates its hormone-dependent interaction with several nuclear receptors. It functions as a molecular scaffold that recruits several proteins that function in transcriptional repression. Remarkably, although the two proteins share only very limited homology, LCoR and another NR box-containing corepressor RIP140 recruit similar cofactors implicated in transcriptional repression, suggesting many parallels in their mechanisms of action. Corepressors such as LCoR and RIP140 may function in negative feedback loops to attenuate hormone-induced transactivation, act more transiently as part of a cycle of cofactors recruited to target promoters by ligand-bound receptors, or function in hormone-induced target gene repression.

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Year:  2004        PMID: 15193453     DOI: 10.1016/S0083-6729(04)68004-6

Source DB:  PubMed          Journal:  Vitam Horm        ISSN: 0083-6729            Impact factor:   3.421


  27 in total

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Review 7.  Deconstructing repression: evolving models of co-repressor action.

Authors:  Valentina Perissi; Kristen Jepsen; Christopher K Glass; Michael G Rosenfeld
Journal:  Nat Rev Genet       Date:  2010-02       Impact factor: 53.242

Review 8.  PPARalpha: energy combustion, hypolipidemia, inflammation and cancer.

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Journal:  Nucl Recept Signal       Date:  2010-04-16

9.  Inhibition of cyclin D1 expression by androgen receptor in breast cancer cells--identification of a novel androgen response element.

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Journal:  Nucleic Acids Res       Date:  2010-04-26       Impact factor: 16.971

10.  ASXL1 represses retinoic acid receptor-mediated transcription through associating with HP1 and LSD1.

Authors:  Sang-Wang Lee; Yang-Sook Cho; Jung-Min Na; Ui-Hyun Park; Myengmo Kang; Eun-Joo Kim; Soo-Jong Um
Journal:  J Biol Chem       Date:  2009-10-31       Impact factor: 5.157

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