[No authors listed]
The synthesis and secretion of surfactant proteins (SPs) is an important sign of lung maturation. Furthermore, the morbidity of lung developmental diseases, including respiratory distress syndrome and bronchopulmonary dysplasia which are mainly caused by immature lung development and lack of SPs, is increasing. As is well known, multiple microRNAs (miRs/miRNAs) are able to influence lung development via numerous different signaling pathways. However, few studies examine the association between the miRNAs and lung developmental diseases. A previous study has demonstrated that miRâ431 was significantly (F=33.49; P<0.001) downregulated in the lung tissues of SpragueâDawley rats at 3 time points, embryonic day 19, embryonic day 21 and postnatal day 3. The present study reported that the regulation of miRâ431 may influence the expression of SPs. Thus, the further potential mechanisms of miRâ431 in negatively regulating lung development were examined in the present study. Stable A549 cell lines overexpressing or knocking down SMAD family member 4 (SMAD4) transfected with miRâ431 overexpressed or knocked down, and their control groups were established. Subsequently, the expression of bone morphogenetic protein 4 (BMP4), SMAD4 and SPs (SPâA, SPâB and SPâC) at the RNA and protein levels were validated respectively by reverse transcription quantitative PCR and western blotting. miRâ431 exhibited a decreased expression, while BMP4 and SPs exhibited increased expression at the mRNA and protein levels in the SMAD4 knockdown group. Meanwhile, the expression of SPs were reduced in the SMAD4âknockdown group via overexpressing miRâ431 and increased in the SMAD4âoverexpression group via inhibiting miRâ431. The present results indicate that SMAD4 negatively regulates the expression of SPs, and that miRâ431 negatively regulates the expression of SPs through inhibiting the BMP4/activin/transforming growth factorâβ signaling pathway by targeting SMAD4.
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