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Loss of Hepatic Oscillatory Fed microRNAs Abrogates Refed Transition and Causes Liver Dysfunctions.

Cell Rep. 2019-02; 
ManiyadathBabukrishna,ChattopadhyayTandrika,VermaSrikant,KumariSujata,KulkarniPrineeta,BanerjeeKushal,LazarusAsmitha,KokaneSaurabh S,ShettyTrupti,AnamikaKrishanpal,Kolthur-SeetharamU
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Gene Synthesis pAdTrack-miRsponge construct was generated by cloning 6x anti-sense sequences of let-7i, 7g, miR-221 and 222 downstream to firefly luciferase gene. Generation of miR-sponge construct was outsourced to GenScript Inc. Get A Quote

摘要

Inability to mediate fed-fast transitions in the liver is known to cause metabolic dysfunctions and diseases. Intuitively, a failure to inhibit futile translation of state-specific transcripts during fed-fast cycles would abrogate dynamic physiological transitions. Here, we have discovered hepatic fed microRNAs that target fasting-induced genes and are essential for a refed transition. Our findings highlight the role of these fed microRNAs in orchestrating system-level control over liver physiology and whole-body energetics. By targeting SIRT1, PGC1α, and their downstream genes, fed microRNAs regulate metabolic and mitochondrial pathways. MicroRNA expression, processing, and RISC loading oscillat... More

关键词

PGC1α,SIRT1,energetics,fast,fatty acid oxidation,fed,gluconeogenesis,liver,microRNA,mitochon