Simvastatin profoundly impairs energy metabolism in primary human muscle cells
Objectives: Simvastatin use is associated with muscular side effects, and i ncreased risk for type 2 diabetes (T2D). In clinical use, simvastatin is administered in inactive lipophilic lactone-form, which is then converted to active acid-form in the body. Here, we have investigated if lactone- and a...
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Bioscientifica
2020-12-01
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| Series: | Endocrine Connections |
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doaj-2f3ff45311eb4ccabbe4a29bbff0a8ce2020-12-14T06:00:36ZengBioscientificaEndocrine Connections2049-36142049-36142020-12-0191111031113https://doi.org/10.1530/EC-20-0444Simvastatin profoundly impairs energy metabolism in primary human muscle cellsSelina Mäkinen0Neeta Datta1Yen H Nguyen2Petro Kyrylenko3Markku Laakso4Heikki A Koistinen5Minerva Foundation Institute for Medical Research, Helsinki, Finland; Department of Medicine, University of Helsinki, Helsinki University Central Hospital, Helsinki, FinlandMinerva Foundation Institute for Medical Research, Helsinki, Finland; Department of Medicine, University of Helsinki, Helsinki University Central Hospital, Helsinki, FinlandMinerva Foundation Institute for Medical Research, Helsinki, Finland; Department of Medicine, University of Helsinki, Helsinki University Central Hospital, Helsinki, FinlandMinerva Foundation Institute for Medical Research, Helsinki, Finland; Department of Medicine, University of Helsinki, Helsinki University Central Hospital, Helsinki, FinlandInstitute of Clinical Medicine, Internal Medicine, University of Eastern Finland, Kuopio, FinlandMinerva Foundation Institute for Medical Research, Helsinki, Finland; Department of Medicine, University of Helsinki, Helsinki University Central Hospital, Helsinki, FinlandObjectives: Simvastatin use is associated with muscular side effects, and i ncreased risk for type 2 diabetes (T2D). In clinical use, simvastatin is administered in inactive lipophilic lactone-form, which is then converted to active acid-form in the body. Here, we have investigated if lactone- and acid-form simvastatin diffe rentially affect glucose metabolism and mitochondrial respiration in primary human skeletal muscle cells. Methods: Muscle cells were exposed separately to lactone- and acid-form simvastatin for 48 h. After pre-exposure, glucose uptake and glycogen synthesis were measured using radioactive tracers; insulin signalling was detected with Western blotting; and glycolysis, mitochondrial oxygen consumption and ATP production were measured with Seahorse XFe96 analyzer. Results: Lactone-form simvastatin increased glucose uptake and glycogen synthesis, whereas acid-form simvastatin did not affect glucose uptake and decreased glycogen synthesis. Phosphorylation of insulin signalling targets Akt substrate 160 kDa (AS160) and glycogen synthase kinase 3β (GSK3β) was upregulated with lactone-, but not with acid-form simvastatin. Exposure to both forms of simvastatin led to a decrease in glycolysis and glycolytic capacity, as well as to a decrease in mitochondrial respiration and ATP production. Conclusions: These data suggest that lactone- and acid-forms of simvastatin exhibit differential effects on non-oxidative glucose metabolism as lacto ne-form increases and acid-form impairs glucose storage into glycogen, suggesting impaired insulin sensitivity in response to acid-form simvastatin. Both forms profoundly impair oxidative glucose metabolism and energy production in human skeletal muscle cells . These effects may contribute to muscular side effects and risk for T2D observed wi th simvastatin use. https://ec.bioscientifica.com/view/journals/ec/9/11/EC-20-0444.xmlatp productionglucose uptakeglycogen synthesisglycolysishmg-coa reductase inhibitorinsulin resistancemitochondrial respirationsimvastatinskeletal muscle |
| collection |
DOAJ |
| language |
English |
| format |
Article |
| sources |
DOAJ |
| author |
Selina Mäkinen Neeta Datta Yen H Nguyen Petro Kyrylenko Markku Laakso Heikki A Koistinen |
| spellingShingle |
Selina Mäkinen Neeta Datta Yen H Nguyen Petro Kyrylenko Markku Laakso Heikki A Koistinen Simvastatin profoundly impairs energy metabolism in primary human muscle cells Endocrine Connections atp production glucose uptake glycogen synthesis glycolysis hmg-coa reductase inhibitor insulin resistance mitochondrial respiration simvastatin skeletal muscle |
| author_facet |
Selina Mäkinen Neeta Datta Yen H Nguyen Petro Kyrylenko Markku Laakso Heikki A Koistinen |
| author_sort |
Selina Mäkinen |
| title |
Simvastatin profoundly impairs energy metabolism in primary human muscle cells |
| title_short |
Simvastatin profoundly impairs energy metabolism in primary human muscle cells |
| title_full |
Simvastatin profoundly impairs energy metabolism in primary human muscle cells |
| title_fullStr |
Simvastatin profoundly impairs energy metabolism in primary human muscle cells |
| title_full_unstemmed |
Simvastatin profoundly impairs energy metabolism in primary human muscle cells |
| title_sort |
simvastatin profoundly impairs energy metabolism in primary human muscle cells |
| publisher |
Bioscientifica |
| series |
Endocrine Connections |
| issn |
2049-3614 2049-3614 |
| publishDate |
2020-12-01 |
| description |
Objectives: Simvastatin use is associated with muscular side effects, and i ncreased risk for type 2 diabetes (T2D). In clinical use, simvastatin is administered in inactive lipophilic lactone-form, which is then converted to active acid-form in the body. Here, we have investigated if lactone- and acid-form simvastatin diffe rentially affect glucose metabolism and mitochondrial respiration in primary human skeletal muscle cells.
Methods: Muscle cells were exposed separately to lactone- and acid-form simvastatin for 48 h. After pre-exposure, glucose uptake and glycogen synthesis were measured using radioactive tracers; insulin signalling was detected with Western blotting; and glycolysis, mitochondrial oxygen consumption and ATP production were measured with Seahorse XFe96 analyzer.
Results: Lactone-form simvastatin increased glucose uptake and glycogen synthesis, whereas acid-form simvastatin did not affect glucose uptake and decreased glycogen synthesis. Phosphorylation of insulin signalling targets Akt substrate 160 kDa (AS160) and glycogen synthase kinase 3β (GSK3β) was upregulated with lactone-, but not with acid-form simvastatin. Exposure to both forms of simvastatin led to a decrease in glycolysis and glycolytic capacity, as well as to a decrease in mitochondrial respiration and ATP production.
Conclusions: These data suggest that lactone- and acid-forms of simvastatin exhibit differential effects on non-oxidative glucose metabolism as lacto ne-form increases and acid-form impairs glucose storage into glycogen, suggesting impaired insulin sensitivity in response to acid-form simvastatin. Both forms profoundly impair oxidative glucose metabolism and energy production in human skeletal muscle cells . These effects may contribute to muscular side effects and risk for T2D observed wi th simvastatin use.
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| topic |
atp production glucose uptake glycogen synthesis glycolysis hmg-coa reductase inhibitor insulin resistance mitochondrial respiration simvastatin skeletal muscle |
| url |
https://ec.bioscientifica.com/view/journals/ec/9/11/EC-20-0444.xml |
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