| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 5946484 | Atherosclerosis | 2014 | 11 Pages |
â¢Highly conserved miR-27a/b can directly target the 3â² UTR of ABCA1, LPL, ACAT1.â¢miR-27a/b can regulate the function of LPL, CD36, apoA-1, LPL, ABCA1 and ACAT1.â¢miR-27a/b affects efflux, influx, esterification and hydrolysis of cholesterol.
RationaleMacrophage cholesterol homeostasis maintenance is the result of a balance between influx, endogenous synthesis, esterification/hydrolysis and efflux. Excessive accumulation of cholesterol leads to foam cell formation, which is the major pathology of atherosclerosis. Previous studies have shown that miR-27 (miR-27a and miR-27b) may play a key role in the progression of atherosclerosis.ObjectiveWe set out to investigate the molecular mechanisms of miR-27a/b in intracellular cholesterol homeostasis.Methods and resultsIn the present study, our results have shown that the miR-27 family is highly conserved during evolution, present in mammals and directly targets the 3â² UTR of ABCA1, LPL, and ACAT1. apoA1, ABCG1 and SR-B1 lacking miR-27 bind sites should not be influenced by miR-27 directly. miR-27a and miR-27b directly regulated the expression of endogenous ABCA1 in different cells. Treatment with miR-27a and miR-27b mimics reduced apoA1-mediated cholesterol efflux by 33.08% and 44.61% in THP-1 cells, respectively. miR-27a/b also regulated HDL-mediated cholesterol efflux in THP-1 macrophages and affected the expression of apoA1 in HepG2 cells. However, miR-27a/b had no effect on total cellular cholesterol accumulation, but regulated the levels of cellular free cholesterol and cholesterol ester. We further found that miR-27a/b regulated the expression of LPL and CD36, and then affected the ability of THP-1 macrophages to uptake Dil-oxLDL. Finally, we identified that miR-27a/b regulated cholesterol ester formation by targeting ACAT1 in THP-1 macrophages.ConclusionThese findings indicate that miR-27a/b affects the efflux, influx, esterification and hydrolysis of cellular cholesterol by regulating the expression of ABCA1, apoA1, LPL, CD36 and ACAT1.
