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A Pleiotropic Role for the Orphan Nuclear Receptor Small Heterodimer Partner in Lipid Homeostasis and Metabolic Pathways
Author(s) -
Gabriella Garruti,
Helen H. Wang,
Leonilde Bonfrate,
Ornella de Bari,
David Q.H. Wang,
Piero Portincasa
Publication year - 2012
Publication title -
journal of lipids
Language(s) - English
Resource type - Journals
eISSN - 2090-3030
pISSN - 2090-3049
DOI - 10.1155/2012/304292
Subject(s) - small heterodimer partner , nuclear receptor , transcription factor , farnesoid x receptor , coactivator , regulator , glucose homeostasis , microbiology and biotechnology , biology , energy homeostasis , function (biology) , neuron derived orphan receptor 1 , biochemistry , bioinformatics , receptor , gene , insulin resistance , insulin , endocrinology
Nuclear receptors (NRs) comprise one of the most abundant classes of transcriptional regulators of metabolic diseases and have emerged as promising pharmaceutical targets. Small heterodimer partner (SHP; NR0B2) is a unique orphan NR lacking a DNA-binding domain but contains a putative ligand-binding domain. SHP is a transcriptional regulator affecting multiple key biological functions and metabolic processes including cholesterol, bile acid, and fatty acid metabolism, as well as reproductive biology and glucose-energy homeostasis. About half of all mammalian NRs and several transcriptional coregulators can interact with SHP. The SHP-mediated repression of target transcription factors includes at least three mechanisms including direct interference with the C-terminal activation function 2 (AF2) coactivator domains of NRs, recruitment of corepressors, or direct interaction with the surface of NR/transcription factors. Future research must focus on synthetic ligands acting on SHP as a potential therapeutic target in a series of metabolic abnormalities. Current understanding about the pleiotropic role of SHP is examined in this paper, and principal metabolic aspects connected with SHP function will be also discussed.

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