Effects of statins on the secretion of human serum albumin in cultured HepG2 cells

被引:0
作者
Chung-Eun Ha
Ji-Sook Ha
Andre G Theriault
Nadhipuram V Bhagavan
机构
[1] University of Hawaii at Manoa,Department of Native Hawaiian Health, John A. Burns School of Medicine
[2] University of Hawaii at Manoa,Department of Anatomy, Biochemistry, & Physiology, John A. Burns School of Medicine
[3] University of Hawaii at Manoa,Department of Medical Technology, John A. Burns School of Medicine
来源
Journal of Biomedical Science | / 16卷
关键词
Simvastatin; Human Serum Albumin; HepG2 Cell; Pravastatin; Lovastatin;
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摘要
Statins reduce cholesterol biosynthesis by inhibiting HMG-CoA reductase and thereby lower total cholesterol and LDL cholesterol levels in serum, which in turn lower the incidence of cardiovascular disease (CVD). Statins are also known to modulate various cellular functions such as gene expression, cell proliferation, and programmed cell death through inhibition of downstream intermediates in cholesterol synthesis. In this study, we have investigated the possible effects of statins on the secretion of serum albumin from cultured HepG2 cells since high levels of serum albumin are associated with reduced risks for CVD and statins are effective in lowering the risk of CVD through other effects in addition to their effects on serum total cholesterol and LDL cholesterol levels, known as pleiotropic effects. Our results showed that simvastatin increased HSA secretion up to 32.3% compared to the control group. Among 3 statin analogs we tested, simvastatin exhibited the highest stimulatory effects on HSA secretion compared to the control group. Our study also showed that the increased HSA secretions from HepG2 cells by simvastatin treatments were due to the increased rate of HSA synthesis, not due to the reduced posttranslational degradation rate of HSA. Our finding suggests another added benefit of statins' treatments in preventing CVD through stimulation of HSA biosynthesis.
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