Literature DB >> 16003294

High-dose statins and skeletal muscle metabolism in humans: a randomized, controlled trial.

Hannu Päivä1, Karin M Thelen, Rudy Van Coster, Joél Smet, Boel De Paepe, Kari M Mattila, Juha Laakso, Terho Lehtimäki, Klaus von Bergmann, Dieter Lütjohann, Reijo Laaksonen.   

Abstract

BACKGROUND: Myopathy, probably caused by 3-hydroxy-3-methylglutaryl-coenzyme A reductase inhibition in skeletal muscle, rarely occurs in patients taking statins. This study was designed to assess the effect of high-dose statin treatment on cholesterol and ubiquinone metabolism and mitochondrial function in human skeletal muscle.
METHODS: Forty-eight patients with hypercholesterolemia (33 men and 15 women) were randomly assigned to receive 80 mg/d of simvastatin (n = 16), 40 mg/d of atorvastatin (n = 16), or placebo (n = 16) for 8 weeks. Plasma samples and muscle biopsy specimens were obtained at baseline and at the end of the follow-up.
RESULTS: The ratio of plasma lathosterol to cholesterol, a marker of endogenous cholesterol synthesis, decreased significantly by 66% in both statin groups. Muscle campesterol concentrations increased from 21.1 +/- 7.1 nmol/g to 41.2 +/- 27.0 nmol/g in the simvastatin group and from 22.6 +/- 8.6 nmol/g to 40.0 +/- 18.7 nmol/g in the atorvastatin group (P = .005, repeated-measurements ANOVA). The muscle ubiquinone concentration was reduced significantly from 39.7 +/- 13.6 nmol/g to 26.4 +/- 7.9 nmol/g (P = .031, repeated-measurements ANOVA) in the simvastatin group, but no reduction was observed in the atorvastatin or placebo group. Respiratory chain enzyme activities were assessed in 6 patients taking simvastatin with markedly reduced muscle ubiquinone and in matched subjects selected from the atorvastatin (n = 6) and placebo (n = 6) groups. Respiratory chain enzyme and citrate synthase activities were reduced in the patients taking simvastatin.
CONCLUSIONS: High-dose statin treatment leads to changes in the skeletal muscle sterol metabolism. Furthermore, aggressive statin treatment may affect mitochondrial volume.

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Year:  2005        PMID: 16003294     DOI: 10.1016/j.clpt.2005.03.006

Source DB:  PubMed          Journal:  Clin Pharmacol Ther        ISSN: 0009-9236            Impact factor:   6.875


  71 in total

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Authors:  Emilie Mas; Trevor A Mori
Journal:  Curr Atheroscler Rep       Date:  2010-11       Impact factor: 5.113

2.  Gene expression in skeletal muscle of coronary artery disease patients after concentric and eccentric endurance training.

Authors:  J Zoll; R Steiner; K Meyer; M Vogt; H Hoppeler; M Flück
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3.  Statin myopathy: incidence, risk factors, and pathophysiology.

Authors:  Kimberly A Sewright; Priscilla M Clarkson; Paul D Thompson
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4.  Coenzyme q10 and statin-induced mitochondrial dysfunction.

Authors:  Richard Deichmann; Carl Lavie; Samuel Andrews
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5.  Apolipoprotein A1 regulates coenzyme Q10 absorption, mitochondrial function, and infarct size in a mouse model of myocardial infarction.

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6.  Effects of fluvastatin and coenzyme Q10 on skeletal muscle in normo- and hypercholesterolaemic rats.

Authors:  J Vincze; Á Jenes; M Füzi; J Almássy; R Németh; G Szigeti; B Dienes; Z Gaál; P Szentesi; I Jóna; P Kertai; G Paragh; L Csernoch
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Review 7.  Coenzyme Q10 as Treatment for Statin-Associated Muscle Symptoms-A Good Idea, but….

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Review 8.  Evidence-based management of statin myopathy.

Authors:  Charles R Harper; Terry A Jacobson
Journal:  Curr Atheroscler Rep       Date:  2010-09       Impact factor: 5.113

9.  Statin-associated polymyositis following omeprazole treatment.

Authors:  Rajan Kanth; Milind S Shah; Rafael Medina Flores
Journal:  Clin Med Res       Date:  2013-04-11

10.  Simvastatin impairs exercise training adaptations.

Authors:  Catherine R Mikus; Leryn J Boyle; Sarah J Borengasser; Douglas J Oberlin; Scott P Naples; Justin Fletcher; Grace M Meers; Meghan Ruebel; M Harold Laughlin; Kevin C Dellsperger; Paul J Fadel; John P Thyfault
Journal:  J Am Coll Cardiol       Date:  2013-04-10       Impact factor: 24.094

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