| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2794036 | Cytokine | 2015 | 8 Pages |
•We stimulated hPDLF with H2O2 in the presence/absence of Ilomastat (MMPs inhibitor).•Oxidant conditions increased anti-oxidant enzymes, cytokines and MMPs.•Oxidant conditions favored cell migration in a MMP-dependent fashion.•Ilomastat modified the effects of H2O2 over cytokine levels and reduced cell migration.•There is a bidirectional regulation system between MMPs and cytokines.
Periodontitis is a highly prevalent infectious disease characterized by the progressive inflammatory destruction of tooth-supporting structures, leading to tooth loss. The underling molecular mechanisms of the disease are incompletely understood, precluding the development of more efficient screening, diagnostic and therapeutic approaches. We investigated the interrelation of three known effector mechanisms of the cellular response to periodontal infection, namely reactive oxygen species (ROS), matrix metalloproteinases (MMPs) and cytokines in primary cell cultures of human periodontal ligament fibroblast (hPDLF). We demonstrated that ROS increase the activity/levels of gelatinolytic MMPs, and stimulate cytokine secretion in hPDLF. Additionally, we proved that MMPs possesses immune modulatory capacity, regulating the secreted levels of cytokines in ROS-stimulated hPDLF cultures. This evidence provides further insight in the molecular pathogenesis of periodontitis, contributing to the future development of more effective therapies.
