ESRP2-microRNA-122 axis directs the postnatal onset of liver polyploidization and maturation.
Sushant BangruJackie ChenNicholas BakerDiptatanu DasUllas V ChembazhiJessica M DerhamSandip ChorghadeWaqar ArifFrances AlencastroAndrew W DuncanRuss P CarstensAuinash KalsotraPublished in: bioRxiv : the preprint server for biology (2024)
Hepatocyte 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 interactions in vivo and 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.
Keyphrases
- rna seq
- single cell
- cell proliferation
- long non coding rna
- long noncoding rna
- transcription factor
- liver injury
- preterm infants
- high throughput
- gene expression
- quality improvement
- genome wide
- palliative care
- adipose tissue
- type diabetes
- dna methylation
- binding protein
- insulin resistance
- nucleic acid
- high fat diet induced
- heat shock