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Lipin 1 modulates mRNA splicing during fasting adaptation in liver

Authors :
Wang, H
Chan, TW
Vashisht, AA
Drew, BG
Calkin, AC
Harris, TE
Wohlschlegel, JA
Xiao, X
Reue, K
Wang, H
Chan, TW
Vashisht, AA
Drew, BG
Calkin, AC
Harris, TE
Wohlschlegel, JA
Xiao, X
Reue, K
Publication Year :
2021

Abstract

Lipin 1 regulates cellular lipid homeostasis through roles in glycerolipid synthesis (through phosphatidic acid phosphatase activity) and transcriptional coactivation. Lipin 1-deficient individuals exhibit episodic disease symptoms that are triggered by metabolic stress, such as stress caused by prolonged fasting. We sought to identify critical lipin 1 activities during fasting. We determined that lipin 1 deficiency induces widespread alternative mRNA splicing in liver during fasting, much of which is normalized by refeeding. The role of lipin 1 in mRNA splicing was largely independent of its enzymatic function. We identified interactions between lipin 1 and spliceosome proteins, as well as a requirement for lipin 1 to maintain homeostatic levels of spliceosome small nuclear RNAs and specific RNA splicing factors. In fasted Lpin1-/- liver, we identified a correspondence between alternative splicing of phospholipid biosynthetic enzymes and dysregulated phospholipid levels; splicing patterns and phospholipid levels were partly normalized by feeding. Thus, lipin 1 influences hepatic lipid metabolism through mRNA splicing, as well as through enzymatic and transcriptional activities, and fasting exacerbates the deleterious effects of lipin 1 deficiency on metabolic homeostasis.

Details

Database :
OAIster
Publication Type :
Electronic Resource
Accession number :
edsoai.on1315726073
Document Type :
Electronic Resource