Age‐related mitophagy regulates orthodontic tooth movement by affecting PDLSCs mitochondrial function and RANKL/OPG

Abstract

AbstractA thorough comprehension of age‐related variances in orthodontic tooth movement (OTM) and bone remodeling response to mechanical force holds significant implications for enhancing orthodontic treatment. Mitophagy plays a crucial role in bone metabolism and various age‐related diseases. However, the impact of mitophagy on the bone remodeling process during OTM remains elusive. Using adolescent (6 weeks old) and adult (12 months old) rats, we established OTM models and observed that orthodontic force increased the expression of the mitophagy proteins PTEN‐induced putative kinase 1 (PINK1) and Parkin, as well as the number of tartrate‐resistant acid phosphatase‐positive osteoclasts and osteocalcin‐positive osteoblasts. These biological changes were found to be age‐related. In vitro, compression force loading promoted PINK1/Parkin‐dependent mitophagy in periodontal ligament stem cells (PDLSCs) derived from adolescents (12–16 years old) and adults (25–35 years old). Furthermore, adult PDLSCs exhibited lower levels of mitophagy, impaired mitochondrial function, and a decreased ratio of RANKL/OPG compared to young PDLSCs after compression. Transfection of siRNA confirmed that inhibition of mitophagy in PDLSC resulted in decreased mitochondrial function and reduced RANKL/OPG ratio. Application of mitophagy inducer Urolithin A enhanced bone remodeling and accelerated OTM in rats, while the mitophagy inhibitor Mdivi‐1 had the opposite effect. These findings indicate that force‐stimulated PDLSC mitophagy contributes to alveolar bone remodeling during OTM, and age‐related impairment of mitophagy negatively impacts the PDLSC response to mechanical stimulus. Our findings enhance the understanding of mitochondrial mechanotransduction and offer new targets to tackle current clinical challenges in orthodontic therapy.