Inhibition of cholesterol synthesis by squalene synthase inhibitors does not induce myotoxicity in vitro

Inhibition of cholesterol synthesis by squalene synthase inhibitors does not induce myotoxicity in vitro

The cholesterol-lowering HMG CoA reductase inhibitors (HMGRI), pravastatin and lovastatin, have been associated with skeletal myopathy in humans and in rats. In a previous in vitro study, HMGRI-induced changes in neonatal rat skeletal muscle cells were characterized by reversible inhibition of prote...

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Veröffentlicht in:Toxicology and applied pharmacology 1997-07, Vol.145 (1), p.91-98
Hauptverfasser: FLINT, O. P, MASTERS, B. A, GREGG, R. E, DURHAM, S. K
Format: Artikel
Sprache:eng
Schlagworte:
Analysis of Variance
Animals
Animals, Newborn
Anticholesteremic Agents - toxicity
Biological and medical sciences
Butylamines - pharmacology
Cells, Cultured
Cholesterol - biosynthesis
Diterpenes - metabolism
Diterpenes - pharmacology
Drug toxicity and drugs side effects treatment
Enzyme Inhibitors - toxicity
Farnesol - metabolism
Farnesol - pharmacology
Farnesyl-Diphosphate Farnesyltransferase - antagonists & inhibitors
Farnesyl-Diphosphate Farnesyltransferase - metabolism
Female
Hydroxymethylglutaryl-CoA Reductase Inhibitors
L-Lactate Dehydrogenase - metabolism
Lovastatin - toxicity
Medical sciences
Mevalonic Acid - pharmacology
Muscle, Skeletal - cytology
Muscle, Skeletal - drug effects
Muscle, Skeletal - enzymology
Pharmacology. Drug treatments
Pravastatin - toxicity
Pregnancy
Prodrugs - pharmacology
Protein Biosynthesis
Rats
Rats, Sprague-Dawley
Squalene - metabolism
Squalene - pharmacology
Sulfonic Acids - pharmacology
Toxicity: nervous system and muscle
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Zusammenfassung:The cholesterol-lowering HMG CoA reductase inhibitors (HMGRI), pravastatin and lovastatin, have been associated with skeletal myopathy in humans and in rats. In a previous in vitro study, HMGRI-induced changes in neonatal rat skeletal muscle cells were characterized by reversible inhibition of protein synthesis and loss of differentiated myotubes at concentrations markedly lower than those inducing enzyme leakage. Myotoxicity was determined to be directly related to inhibition of HMG CoA reductase, since mevalonate, the immediate product of HMG CoA reductase metabolism, abrogated the drug-induced changes. Farnesol, geranylgeraniol, and squalene are metabolites of mevalonate. Squalene, formed from farnesol by squalene synthase, is the first metabolite solely committed to cholesterol synthesis. In contrast, geranylgeraniol, formed by the addition of an isoprene group to farnesol, is the first metabolite uncommitted to cholesterol synthesis. The objective of the present study was to determine the role of inhibition of cholesterol synthesis in HMGRI-induced in vitro myotoxicity. HMGRI-treated neonatal rat skeletal muscle cultures were supplemented with farnesol and geranylgeraniol, and in another study, muscle cultures were exposed to two squalene synthase inhibitors (SSI), BMS-187745 and its prodrug ester, BMS-188494. Endpoints evaluated for both studies included protein synthesis ([3H]leucine incorporation), total cellular protein (a measure of cell loss), intra- and extracellular lactate dehydrogenase activity (a measure of membrane integrity), cholesterol biosynthesis ([14C]acetate incorporation), and morphology. HMG CoA reductase inhibitor-induced morphologic changes and inhibition of protein synthesis were significantly ameliorated by supplementation with farnesol and geranylgeraniol. In contrast to HMGRI-induced in vitro myotoxicity, SSI induced an irreversible, minimal cytotoxicity at close to maximum soluble concentrations. These results indicate that depletion of metabolites of geranylgeranyl pyrophosphate, and not inhibition of cholesterol synthesis, is the primary cause of HMG CoA reductase-induced myotoxicity.
ISSN:0041-008X
1096-0333
DOI:10.1006/taap.1997.8131