Recombinant Rat Carbohydrate-responsive element-binding protein (Mlxipl), partial

1. Authors have identified a previously unappreciated negative feedback loop by which glucose-induced ChREBP-beta downregulates ChREBP-alpha-signaling providing new insight into the physiological role of islet ChREBP-beta and into the regulation of glucose-induced gene expression. PMID: 27900263
2. Integrative genomics outlines a biphasic glucose response and a ChREBP-RORgamma axis regulating proliferation in pancreatic beta cells. PMID: 27545881
3. The involvement of ChREBP in FASN promoter histone modification. PMID: 28027934
4. The crystal structure showed that AMP binds directly to the N terminus of ChREBP-alpha2 helix. Our results suggest that AMP inhibits the nuclear localization of ChREBP through an allosteric activation of ChREBP/14-3-3 interactions and not by activation of AMPK. PMID: 26984404
5. Data suggest expression of ChREBPbeta isoform is up-regulated in pancreatic beta-cells in response to elevated glucose (i.e., hyperglycemic conditions); RNA interference of ChREBPbeta prevents beta-cell proliferation in response to hyperglycemia. PMID: 26384380
6. The ChREBP mutant, W130A, did not exhibit HG-induced lipid accumulation and fibrotic proteins, suggesting that the Trp-130 residue in the MCR3 domain is important in the development of glomerulosclerosis. PMID: 24616092
7. ketone bodies play an important role in the regulation of ChREBP activity by restricting ChREBP localization to the cytoplasm, thus inhibiting fat synthesis during periods of ketosis PMID: 23918932
8. Data from pancreatic beta-cell line suggest that glucose-6-phosphate and xylulose-5-phosphate can activate ChREBP transactivity, but their potencies to induce ChREBP transactivity are much lower than that of glucose. PMID: 23257733
9. Glucose, through the transcription factor ChREBP, controls beta cell differentiation from pancreatic progenitors. PMID: 22760788
10. an important mechanism by which importin-alpha and 14-3-3 control movement of ChREBP in and out of the nucleus in response to changes in glucose levels in liver PMID: 21665952
11. ChREBP directly regulates rat Gcgr expression in INS-1E cells. PMID: 22198437
12. The activation and recruitment of ChREBP to several glucose-responsive genes were blocked by 1RH, indicating a general necessity for c-Myc in this process. PMID: 20382893
13. Mlx is an obligatory partner of ChREBP in regulating lipogenic enzyme genes in liver. PMID: 15664996
14. ChREBP.Mlx is the principal transcription factor regulating glucose-responsive genes in the liver and coordinately regulates a family of genes required for glucose utilization and energy storage PMID: 16885160
15. Maximal glucose-induced expression of the L-PK gene in INS-1-derived 832/13 cells involves increased c-Myc abundance, recruitment of c-Myc, Max, and ChREBP to the promoter, and a glucose-stimulated increase in ChREBP transactivation. PMID: 17341548
16. The ChREBP gene contains a cluster of putative transcription factor-binding elements consisting of two specificity protein 1 (Sp1) binding sites, a sterol regulatory element, and two nuclear factor-Y binding sites critical for ChREBP gene transcription. PMID: 17418800
17. ChREBP activity is regulated by complex multisite phosphorylation patterns involving its N-terminal regulatory region PMID: 18215143

Show More

Hide All

KEGG: rno:171078

STRING: 10116.ENSRNOP00000066522

UniGene: Rn.144656