Journal article

The impact of simvastatin on lipidomic markers of cardiovascular risk in human liver cells is secondary to the modulation of intracellular cholesterol

YL Schooneveldt, C Giles, MF Keating, NA Mellett, AW Jurrjens, S Paul, AC Calkin, PJ Meikle

Metabolites | MDPI | Published : 2021

DOI: 10.3390/metabo11060340

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Abstract

Statins are the first-line lipid-lowering therapy for reducing cardiovascular disease (CVD) risk. A plasma lipid ratio of two phospholipids, PI(36:2) and PC(18:0_20:4), was previously identified to explain 58% of the relative CVD risk reduction associated with pravastatin, independent of a change in low-density lipoprotein-cholesterol. This ratio may be a potential biomarker for the treatment effect of statins; however, the underlying mechanisms linking this ratio to CVD risk remain unclear. In this study, we investigated the effect of altered cholesterol conditions on the lipidome of cultured human liver cells (Hep3B). Hep3B cells were treated with simvastatin (5 µM), cyclodextrin (20 mg/mL..

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University of Melbourne Researchers

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Funding Acknowledgements

This work was supported in part by the Victorian Government's Operational Infrastructure Support Program.

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Keywords

Statins
Targeted Lipidomics
Coronary-Heart-Disease
Biochemistry & Molecular Biology
Hepatic Steatosis
Prevention
Cholesterol
Liver Disease
Resistance
Lipid Metabolism
Low-Density Lipoprotein Cholesterol
Cardiovascular Disease
Cardiovascular
Nutrition
Life Sciences & Biomedicine
Heart Disease
Digestive Diseases
Pravastatin
32 Biomedical and Clinical Sciences
3205 Medical Biochemistry and Metabolomics
Atherosclerosis
Arachidonic-Acid
Fatty-Acids
Science & Technology