| Literature DB >> 12791702 |
Larbi Amazit1, Youssef Alj, Rakesh Kumar Tyagi, Anne Chauchereau, Hugues Loosfelt, Christophe Pichon, Jacques Pantel, Emmanuelle Foulon-Guinchard, Philippe Leclerc, Edwin Milgrom, Anne Guiochon-Mantel.
Abstract
Steroid hormone receptors are ligand-stimulated transcription factors that modulate gene transcription by recruiting coregulators to gene promoters. Subcellular localization and dynamic movements of transcription factors have been shown to be one of the major means of regulating their transcriptional activity. In the present report we describe the subcellular localization and the dynamics of intracellular trafficking of steroid receptor coactivator 1 (SRC-1). After its synthesis in the cytoplasm, SRC-1 is imported into the nucleus, where it activates transcription and is subsequently exported back to the cytoplasm. In both the nucleus and cytoplasm, SRC-1 is localized in speckles. The characterization of SRC-1 nuclear localization sequence reveals that it is a classic bipartite signal localized in the N-terminal region of the protein, between amino acids 18 and 36. This sequence is highly conserved within the other members of the p160 family. Additionally, SRC-1 nuclear export is inhibited by leptomycin B. The region involved in its nuclear export is localized between amino acids 990 and 1038. It is an unusually large domain differing from the classic leucine-rich NES sequences. Thus SRC-1 nuclear export involves either an alternate type of NES or is dependent on the interaction of SRC-1 with a protein, which is exported through the crm1/exportin pathway. Overall, the intracellular trafficking of SRC-1 might be a mechanism to regulate the termination of hormone action, the interaction with other signaling pathways in the cytoplasm and its degradation.Entities:
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Year: 2003 PMID: 12791702 DOI: 10.1074/jbc.M300730200
Source DB: PubMed Journal: J Biol Chem ISSN: 0021-9258 Impact factor: 5.157