FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W744364702> ?p ?o ?g. }

• W744364702 abstract "Nuclear receptors (NRs) are ligand-activated transcription factors. They regulate key biological processes including homeostasis of lipophilic molecules, organogenesis, development, and reproduction. The ability of NRs to regulate gene transcription is dependent upon their ability to directly binding to specific enhancer elements within the promoters of their target genes. While NRs directly bind to DNA, they lack the capacity to modify chromatin, unwind DNA, and recruit transcriptional machinery. All of these aforementioned processes represent key steps in the regulation of gene transcription. Therefore, the full functional activity of NRs depends upon their ability to interact with protein cofactors, termed coactivator and corepressor proteins. Metabolic syndrome is an emerging global epidemic characterized by a complex disorder that affects both glucose and lipid metabolism. Peroxisome proliferator-activated receptor-gamma (PPARγ) co-activator-1alpha (PGC-1α) is a coactivator protein that is mainly expressed in tissues that require a high oxidative capacity such as fat, muscle, brain, and liver. PGC-1α plays an important role in regulating key metabolic processes involved in energy homeostasis including gluconeogenesis, mitochondrial biogenesis, adaptive thermogenesis, and βoxidation of fatty acids. PGC-1α accomplishes this feat through its ability to interact with selected NRs and certain other transcription factor types. PGC-1β is the closest homolog of PGC-1α and also shares some similarities with PGC-1α in amino acid sequence, expression pattern, interacting protein partners, target genes, and ii biochemical function. However, these two coactivator proteins also display distinct proerties. For example, PGC-1β mediates hepatic lipogenic program but not gluconeogenesis, whereas PGC-1α plays a key regulatory role in hepatic gluconeogenesis but has no effects upon lipogenesis. We therefore hypothesized that the key biological and functional differences between these two coactivator proteins is due to their distinct protein interaction profile. A comparison of the primary amino acid sequence of PGC-1α and PGC-1β revealed that both proteins contain three NRinteraction motifs (-LXXLL-) with the first two being highly conserved in their Ntermini, respectively. However, PGC-1β contains an additional and unique stretch of amino acid sequence that separates the second and third NR-interaction motif that is absent from PGC-1α. We therefore fused the cDNA encoding this N-terminal region of PGC-1β to the GAL4-DNA binding domain (GAL4-NBT3) and used this protein as ‘bait’ to screen cDNA expression libraries from liver, brain, and embryo using the yeast two hybrid system to identify novel PGC-1β-interacting proteins. Three potential PGC-1β-interacting proteins were identified. The first is a NR protein called COUP-TF1. The second PGC-1β-interacting protein we identified is a protein phosphatase regulatory protein termed PP4R1. The third protein we identified as a PGC-1β-interacting protein is a member of the SWI/SNF family of proteins called BAF60a. We further confirmed the interaction of PGC-1β/PP4R1 and PGC1β/BAF60a in vitro using the GST pull-down assay. In vivo analysis using immunohistochemical methods further confirms the ability of PP4R1 and BAF60a to" @default.
• W744364702 created "2016-06-24" @default.
• W744364702 creator A5028792040 @default.
• W744364702 date "2008-01-01" @default.
• W744364702 modified "2023-09-24" @default.
• W744364702 title "Identification and Biochemical Characterization of PGC-1beta-Interacting Proteins" @default.
• W744364702 cites W134153864 @default.
• W744364702 cites W140425272 @default.
• W744364702 cites W1501286679 @default.
• W744364702 cites W1523158326 @default.
• W744364702 cites W1564289967 @default.
• W744364702 cites W1570612145 @default.
• W744364702 cites W1613446635 @default.
• W744364702 cites W1633325203 @default.
• W744364702 cites W1963739832 @default.
• W744364702 cites W1964876127 @default.
• W744364702 cites W1969369593 @default.
• W744364702 cites W1974220331 @default.
• W744364702 cites W1975600010 @default.
• W744364702 cites W1976998737 @default.
• W744364702 cites W1977000651 @default.
• W744364702 cites W1979026271 @default.
• W744364702 cites W1984668213 @default.
• W744364702 cites W1984793963 @default.
• W744364702 cites W1986946962 @default.
• W744364702 cites W1990755760 @default.
• W744364702 cites W1997312454 @default.
• W744364702 cites W2004988279 @default.
• W744364702 cites W2007980073 @default.
• W744364702 cites W2008632158 @default.
• W744364702 cites W2017011351 @default.
• W744364702 cites W2026833147 @default.
• W744364702 cites W2026901592 @default.
• W744364702 cites W2028053287 @default.
• W744364702 cites W2028980494 @default.
• W744364702 cites W2031877157 @default.
• W744364702 cites W2035747081 @default.
• W744364702 cites W2036639816 @default.
• W744364702 cites W2044495919 @default.
• W744364702 cites W2045497589 @default.
• W744364702 cites W2046079276 @default.
• W744364702 cites W2046566365 @default.
• W744364702 cites W2049652810 @default.
• W744364702 cites W2057145009 @default.
• W744364702 cites W2068972095 @default.
• W744364702 cites W2069853996 @default.
• W744364702 cites W2072062691 @default.
• W744364702 cites W2074442179 @default.
• W744364702 cites W2077528576 @default.
• W744364702 cites W2081472732 @default.
• W744364702 cites W2088086126 @default.
• W744364702 cites W2101797210 @default.
• W744364702 cites W2104360623 @default.
• W744364702 cites W2104389054 @default.
• W744364702 cites W2124155893 @default.
• W744364702 cites W2124612536 @default.
• W744364702 cites W2125407920 @default.
• W744364702 cites W2131144673 @default.
• W744364702 cites W2131354928 @default.
• W744364702 cites W2135716791 @default.
• W744364702 cites W2141789735 @default.
• W744364702 cites W2141956604 @default.
• W744364702 cites W2155045727 @default.
• W744364702 cites W2157199218 @default.
• W744364702 cites W2158088166 @default.
• W744364702 cites W2160769801 @default.
• W744364702 cites W2167569899 @default.
• W744364702 cites W2168681882 @default.
• W744364702 cites W2886534997 @default.
• W744364702 hasPublicationYear "2008" @default.
• W744364702 type Work @default.
• W744364702 sameAs 744364702 @default.
• W744364702 citedByCount "0" @default.
• W744364702 crossrefType "dissertation" @default.
• W744364702 hasAuthorship W744364702A5028792040 @default.
• W744364702 hasConcept C104317684 @default.
• W744364702 hasConcept C124170894 @default.
• W744364702 hasConcept C134018914 @default.
• W744364702 hasConcept C146777309 @default.
• W744364702 hasConcept C187345961 @default.
• W744364702 hasConcept C2777391703 @default.
• W744364702 hasConcept C2779306644 @default.
• W744364702 hasConcept C3018667095 @default.
• W744364702 hasConcept C55493867 @default.
• W744364702 hasConcept C63932345 @default.
• W744364702 hasConcept C77445288 @default.
• W744364702 hasConcept C86339819 @default.
• W744364702 hasConcept C86803240 @default.
• W744364702 hasConcept C95444343 @default.
• W744364702 hasConceptScore W744364702C104317684 @default.
• W744364702 hasConceptScore W744364702C124170894 @default.
• W744364702 hasConceptScore W744364702C134018914 @default.
• W744364702 hasConceptScore W744364702C146777309 @default.
• W744364702 hasConceptScore W744364702C187345961 @default.
• W744364702 hasConceptScore W744364702C2777391703 @default.
• W744364702 hasConceptScore W744364702C2779306644 @default.
• W744364702 hasConceptScore W744364702C3018667095 @default.
• W744364702 hasConceptScore W744364702C55493867 @default.
• W744364702 hasConceptScore W744364702C63932345 @default.
• W744364702 hasConceptScore W744364702C77445288 @default.

• next