MBNL1 regulates programmed postnatal switching between regenerative and differentiated cardiac states.
Logan R J BaileyDarrian BuggIsabella M ReichardtC Dessirée OrtaçJagadambika GunajeRichard JohnsonMichael J MacCossTomoya SakamotoDaniel P KellyMichael RegnierJennifer M DavisPublished in: bioRxiv : the preprint server for biology (2023)
Discovering determinants of cardiomyocyte maturity and the maintenance of differentiated states is critical to both understanding development and potentially reawakening endogenous regenerative programs in adult mammalian hearts as a therapeutic strategy. Here, the RNA binding protein Muscleblind-like 1 (MBNL1) was identified as a critical regulator of cardiomyocyte differentiated states and their regenerative potential through transcriptome-wide control of RNA stability. Targeted MBNL1 overexpression early in development prematurely transitioned cardiomyocytes to hypertrophic growth, hypoplasia, and dysfunction, whereas loss of MBNL1 function increased cardiomyocyte cell cycle entry and proliferation through altered cell cycle inhibitor transcript stability. Moreover, MBNL1-dependent stabilization of the estrogen-related receptor signaling axis was essential for maintaining cardiomyocyte maturity. In accordance with these data, modulating MBNL1 dose tuned the temporal window of cardiac regeneration, where enhanced MBNL1 activity arrested myocyte proliferation, and MBNL1 deletion promoted regenerative states with prolonged myocyte proliferation. Collectively these data suggest MBNL1 acts as a transcriptome-wide switch between regenerative and mature myocyte states postnatally and throughout adulthood.
Keyphrases
- cell cycle
- stem cells
- mesenchymal stem cells
- cell proliferation
- cell therapy
- tissue engineering
- signaling pathway
- angiotensin ii
- electronic health record
- high glucose
- left ventricular
- rna seq
- gene expression
- single cell
- heart failure
- oxidative stress
- binding protein
- depressive symptoms
- preterm infants
- dna methylation
- machine learning