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Publication : Specific ablation of the NCoR corepressor δ splice variant reveals alternative RNA splicing as a key regulator of hepatic metabolism.

First Author  Goodson ML Year  2020
Journal  PLoS One Volume  15
Issue  10 Pages  e0241238
PubMed ID  33104749 Mgi Jnum  J:296896
Mgi Id  MGI:6471495 Doi  10.1371/journal.pone.0241238
Citation  Goodson ML, et al. (2020) Specific ablation of the NCoR corepressor delta splice variant reveals alternative RNA splicing as a key regulator of hepatic metabolism. PLoS One 15(10):e0241238
abstractText  The NCoR corepressor plays critical roles in mediating transcriptional repression by both nuclear receptors and non-receptor transcription factors. Alternative mRNA splicing of NCoR produces a series of variants with differing molecular and biological properties. The NCoRomega splice-variant inhibits adipogenesis whereas the NCoRdelta splice-variant promotes it, and mice bearing a splice-specific knockout of NCoRomega display enhanced hepatic steatosis and overall weight gain on a high fat diet as well as a greatly increased resistance to diet-induced glucose intolerance. We report here that the reciprocal NCoRdelta splice-specific knock-out mice display the contrary phenotypes of reduced hepatic steatosis and reduced weight gain relative to the NCoRomega-/- mice. The NCoRdelta-/- mice also fail to demonstrate the strong resistance to diet-induced glucose intolerance exhibited by the NCoRomega-/- animals. The NCoR delta and omega variants possess both unique and shared transcriptional targets, with expression of certain hepatic genes affected in opposite directions in the two mutants, others altered in one but not the other genotype, and yet others changed in parallel in both NCoRdelta-/- and NCoRomega-/- animals versus WT. Gene set expression analysis (GSEA) identified a series of lipid, carbohydrate, and amino acid metabolic pathways that are likely to contribute to their distinct steatosis and glucose tolerance phenotypes. We conclude that alternative-splicing of the NCoR corepressor plays a key role in the regulation of hepatic energy storage and utilization, with the NCoRdelta and NCoRomega variants exerting both opposing and shared functions in many aspects of this phenomenon and in the organism as a whole.
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