[No authors listed]
The elucidation of the underlying molecular mechanism of H2O2âinduced adipocyte differentiation in mesenchymal stem cells (MSCs) is important for the development of treatments for metabolic diseases. The aim of the present study was to identify microRNA (miR)â330â5p, which targets retinoid X receptor γ (RXRγ) and to determine the function of H2O2âinduced adipogenic differentiation of MSCs. During differentiation of MSCs into adipocytes induced by H2O2, miRâ330â5p expression was decreased with a concomitant increase in RXRγ expression. A luciferase assay with RXRγ 3'âuntranslated region (UTR) reporter plasmid, including the miRâ330â5pâbinding sequences, identified that the introduction of miRâ330â5p decreases luciferase activity. However, it did not affect the activity of mutated RXRγ 3'âUTR reporter. Enforced expression of miRâ330â5p significantly inhibited adipocyte differentiation by decreasing RXRγ mRNA and protein levels. In contrast, inhibition of the endogenous miRâ330â5p promoted the formation of lipid droplets by rescuing RXRγ expression. Furthermore, the effects of inhibition of RXRγ were similar to those of overexpression of miRâ330â5p on H2O2âinduced adipogenic differentiation from MSCs. miRâ330â5p inhibits H2O2âinduced adipogenic differentiation of MSCs, and this is dependent on RXRγ. Taken together, the results of the present study revealed that miRâ330â5p acts as a critical regulator of RXRγ, and is able to determinate the fate of MSCs to differentiate into adipocytes. This suggests that miRâ330â5p and RXRγ may be target molecules for controlling metabolic diseases.
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