
Examines mitochondrial energy imbalance as a driver of fibroblast senescence and tissue-specific inflammatory aging, illustrated with periodontal ligament fibroblasts.
Key Takeaways
- Fibroblasts are key effectors of tissue remodeling and inflammation
- Researchers must first characterize the tissue-specific mitochondrial signatures of SASP
- Although the regulatory mechanisms of SASP have been extensively investigated
