Abstract
AbstractBone metabolism is highly regulated, and microRNAs (miR) can contribute to this process. Among them, miR-125b is well-known to enhance osteoporosis and reduce osteogenic differentiation of human mesenchymal stem cells (hMSCs). In this work we aim to evaluate and understand how miR-125b modulates mineralization of hMSCs in two differentin vitromodels. Cells were cultured in dexamethasone or calcium medium and transfected with miR-125b mimic. Exposure to dexamethasone or calcium medium increased mineralization of hMSCs and was associated with decreased miR-125b expression. Transfection of miR-125b mimic in dexamethasone-treated cells increased mineralization while it decreased it in calcium-treated cells. Levels of osteogenic markers presented the same difference. We identified STAT3, p53 and RUNX2 as direct targets of miR-125b in hMSCs. While these targets remained identical in both treatments, their modulation after transfection was different. We showed that miR-125b mimicking differentially modulated the expression of the miR-199a/214 cluster, probably via STAT3/miR-199a/214, and p53/miR-214 pathways. In conclusion, miR-125b affinity for targets implicated in bone remodeling changed depending on thein vitromodels used to induce mineralization and led to opposite physiological effect. This works shows the complexity of drugs such as dexamethasone and opens the door for newin vitromodels of mineralization.
Publisher
Cold Spring Harbor Laboratory