MAST4 regulates stem cell maintenance with DLX3 for epithelial development and amelogenesis.
Dong-Joon LeePyunggang KimHyun-Yi KimJinah ParkSeung-Jun LeeHaein AnJin Sun HeoMin-Jung LeeHayato OhshimaSeiya MizunoSatoru TakahashiHan-Sung JungSeong-Jin KimPublished in: Experimental & molecular medicine (2024)
The asymmetric division of stem cells permits the maintenance of the cell population and differentiation for harmonious progress. Developing mouse incisors allows inspection of the role of the stem cell niche to provide specific insights into essential developmental phases. Microtubule-associated serine/threonine kinase family member 4 (Mast4) knockout (KO) mice showed abnormal incisor development with low hardness, as the size of the apical bud was decreased and preameloblasts were shifted to the apical side, resulting in amelogenesis imperfecta. In addition, Mast4 KO incisors showed abnormal enamel maturation, and stem cell maintenance was inhibited as amelogenesis was accelerated with Wnt signal downregulation. Distal-Less Homeobox 3 (DLX3), a critical factor in tooth amelogenesis, is considered to be responsible for the development of amelogenesis imperfecta in humans. MAST4 directly binds to DLX3 and induces phosphorylation at three residues within the nuclear localization site (NLS) that promotes the nuclear translocation of DLX3. MAST4-mediated phosphorylation of DLX3 ultimately controls the transcription of DLX3 target genes, which are carbonic anhydrase and ion transporter genes involved in the pH regulation process during ameloblast maturation. Taken together, our data reveal a novel role for MAST4 as a critical regulator of the entire amelogenesis process through its control of Wnt signaling and DLX3 transcriptional activity.
Keyphrases
- stem cells
- protein kinase
- cell therapy
- transcription factor
- single cell
- gene expression
- cell proliferation
- type diabetes
- metabolic syndrome
- bone marrow
- electronic health record
- artificial intelligence
- signaling pathway
- minimally invasive
- skeletal muscle
- dna methylation
- adipose tissue
- big data
- wild type
- genome wide analysis