ESRP2-microRNA-122 axis directs the postnatal onset of liver polyploidization and maturation

Author:

Bangru SushantORCID,Chen Jackie,Baker Nicholas,Das Diptatanu,Chembazhi Ullas V.,Derham Jessica M.,Chorghade Sandip,Arif Waqar,Alencastro Frances,Duncan Andrew W.,Carstens Russ P.,Kalsotra AuinashORCID

Abstract

SUMMARYHepatocyte polyploidy and maturity are critical to acquiring specialized liver functions. Multiple intra- and extracellular factors influence ploidy, but how they cooperate temporally to steer liver polyploidization and maturation or how post-transcriptional mechanisms integrate into these paradigms is unknown. Here, we identified an important regulatory hierarchy in which postnatal activation of Epithelial-Splicing-Regulatory-Protein-2 (ESRP2) stimulates biogenesis of liver-specific microRNA (miR-122), thereby facilitating polyploidization, maturation, and functional competence of hepatocytes. By determining transcriptome-wide protein-RNA interactionsin vivoand integrating them with single-cell and bulk hepatocyte RNA-seq datasets, we delineate an ESRP2-driven RNA processing program that drives sequential replacement of fetal-to-adult transcript isoforms. Specifically, ESRP2 binds the primary miR-122 host gene transcript to promote its processing/biogenesis. Combining constitutive and inducible ESRP2 gain- and loss-of-function mice models with miR-122 rescue experiments, we demonstrate that timed activation of ESRP2 augments miR-122-driven program of cytokinesis failure, ensuring proper onset and extent of hepatocyte polyploidization.

Publisher

Cold Spring Harbor Laboratory

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