MLL1 is required for PAX7 expression and satellite cell self-renewal in mice.
Gregory C AddicksCaroline E BrunMarie-Claude SincennesJohn SaberChristopher J PorterA Francis StewartPatricia ErnstMichael A RudnickiPublished in: Nature communications (2019)
PAX7 is a paired-homeobox transcription factor that specifies the myogenic identity of muscle stem cells and acts as a nodal factor by stimulating proliferation while inhibiting differentiation. We previously found that PAX7 recruits the H3K4 methyltransferases MLL1/2 to epigenetically activate target genes. Here we report that in the absence of Mll1, myoblasts exhibit reduced H3K4me3 at both Pax7 and Myf5 promoters and reduced Pax7 and Myf5 expression. Mll1-deficient myoblasts fail to proliferate but retain their differentiation potential, while deletion of Mll2 had no discernable effect. Re-expression of PAX7 in committed Mll1 cKO myoblasts restored H3K4me3 enrichment at the Myf5 promoter and Myf5 expression. Deletion of Mll1 in satellite cells reduced satellite cell proliferation and self-renewal, and significantly impaired skeletal muscle regeneration. Pax7 expression was unaffected in quiescent satellite cells but was markedly downregulated following satellite cell activation. Therefore, MLL1 is required for PAX7 expression and satellite cell function in vivo. Furthermore, PAX7, but not MLL1, is required for Myf5 transcriptional activation in committed myoblasts.
Keyphrases
- acute myeloid leukemia
- poor prognosis
- stem cells
- skeletal muscle
- transcription factor
- protein protein
- cell proliferation
- binding protein
- induced apoptosis
- gene expression
- long non coding rna
- signaling pathway
- cell therapy
- type diabetes
- metabolic syndrome
- small molecule
- radiation therapy
- risk assessment
- squamous cell carcinoma
- genome wide
- cell death
- cell cycle
- pi k akt
- climate change
- long noncoding rna
- locally advanced