KDM3A inhibition attenuates high concentration insulinâinduced vascular smooth muscle cell injury by suppressing MAPK/NFâκB pathways.
[No authors listed]
摘要
Previous studies have indicated that lysine (K)âspecific demethylase 3A (KDM3A) is associated with diverse diabetesâassociated cardiovascular complications in response to high glucose levels. However, the effects of KDM3A on the pathological progression of cardiovascular injuries in response to high insulin levels remain unknown. The present study aimed to explore whether KDM3A knockdown may attenuate high insulinâinduced vascular smooth muscle cell (VSMC) dysfunction, and to further investigate the underlying mechanisms. Primary VSMCs were isolated from the thoracic aorta of SpragueâDawley rats. Lentiviral vectors encoding controlâsmall interfering (si)RNA or KDM3AâsiRNA were transduced into VSMCs for 72 h, and cells were subsequently incubated in medium containing 100 nM insulin for a further 5 days. Cellular proli-feration, migration and apoptosis were measured by Cell Counting kitâ8, Transwell chamber assay and flow cytometry, respectively. Reactive oxygen were detected using the dihydroethidium fluorescent probe. The mRNA expression levels of interleukinâ6 and monocyte chemotactic proteinâ1 were measured by reverse transcriptionâquantitative polymerase chain reaction. Furthermore, the protein expression levels of KDM3A, mitogenâactivated protein kinases (MAPKs), nuclear factor (NF)âκB/p65, Bâcell lymphoma 2 (Bclâ2)âassociated X protein and Bclâ2 were evaluated by west-ern blotting. Lentivirus transduction with KDM3AâsiRNA markedly reduced the elevated expression of KDM3A induced by high insulin stimulation in VSMCs. In addition, inhibition of KDM3A significantly ameliorated insulinâinduced VSMC proliferation and migration, which was accompanied by decreased levels, cell apoptosis and inflammatory cytokine levels. Furthermore, KDM3A gene silencing mitigated phosphorylation of MAPKs and NFâκB/p65 activation. In conclusion, KDM3A inhibition may exert numerous protective effects on high insulinâstimulated VSMCs, and the underlying mechanisms may be partly associated with inactivation of MAPK/NFâκB signaling pathways.
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基因功能
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原始数据
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