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Open the LID: LXRα regulates ChREBPα transactivity in a target gene-specific manner through an agonist-modulated LBD-LID interaction

biorxiv. 2019; 
Qiong Fan, Rikke C. Nørgaard, Ivar Grytten, Cecilie M. Ness, Christin Lucas, Kristin Vekterud, Helen Soedling, Jason Matthews, Roza B. Lemma, Odd S. Gabrielsen, Christian Bindesbøll, Stine M. Ulven, Hilde I. Nebb, Line M. Grønning-Wang, Thomas Sæther
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Gene Synthesis The multimerized ChoRE and LXRE reporters: pGL3b-2xChoRE-2xLXRE-10 (ChoRE+LXRE-luc), pGL3b-2xChoRE-10 (ChoRE-only-luc), and pGL3b-2xLXRE-10 (LXRE-only-luc) were constructed in two steps: First, the 136 bp inserts were made by gene synthesis (GenScript, Nanjing, China). Get A Quote

摘要

The cholesterol-sensing nuclear receptor liver X receptor (LXR) and the glucose-sensing transcription factor carbohydrate responsive element-binding protein (ChREBP) are central players in regulating glucose and lipid metabolism in liver. We have previously shown that LXR regulates ChREBP transcription and activity; however, the underlying mechanisms are unclear. In the current study, we demonstrate that LXRα and ChREBPα interact physically, and show a high co-occupancy at regulatory regions in the mouse genome. LXRα co-activates ChREBPα, and regulates ChREBP-specific target genes in vitro and in vivo. This co-activation is dependent on functional recognition elements for ChREBP, but not for LXR, indicat... More

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