Trial finds drug is well tolerated and less likely than other statins to cause muscle-related side effects. Fluvastatin XL, either alone or in combination with ezetimibe, is an effective, well-tolerated, and safe option for lowering LDL cholesterol in patients who can’t tolerate other statins because of muscle-related side effects.
Statin-associated mild to moderate muscle-related side effects such as myalgias, cramping, and weakness are far more common and debilitating in daily practice than suggested by high-profile, highly selective clinical trials. And fluvastatin XL is less likely than other statins to cause these problems. He presented a randomized double-blind placebo-controlled trial restricted to patients forced to discontinue statins other than fluvastatin because of muscle-related side effects.
The results showed 85% of participants could be maintained on fluvastatin XL at 80 mg/day or fluvastatin XL 80 mg plus ezetimibe at 10 mg/day without muscle-related problems. Moreover, the dropout rate owing to muscle-related side effects in the 12-week study was less than 5%, although everyone in the trial had already discontinued another statin for that very reason.
Doctor stressed that they are not talking about myopathy and rhabdomyolysis, serious but rare side effects of statin therapy. He focused on mild to moderate muscle pain, cramping, and weakness. The big randomized trials suggest that prevalence of such problems is 2%-4%, but many clinicians say the figure in everyday practice is much higher.
In the trial at 27 US and European centers, 199 patients with a history of intolerance to statins other than fluvastatin due to muscle-related side effects were randomized to 12 weeks of ezetimibe plus placebo, or both drugs. LDL cholesterol lowering with fluvastatin, with or without ezetimibe, was greater than with ezetimibe alone. Muscle-related side effects in the two fluvastatin arms were slightly lower than with ezetimibe. And when such side effects occurred in patient on fluvastatin alone, they began in the first month, whereas with ezetimibe they started any time during the 3-month trial.
The combination therapy’s effect upon C-reactive protein lowering is difficult to explain but has consistently been seen in other studies of ezetimibe plus various statins. Mean baseline LDL cholesterol in the study cohort was 175 mg/dL. Eighty percent of subjects were high risk by National Cholesterol Education Program (NCEP) criteria. Fluvastatin XL enabled many to reach their NCEP LDL cholesterol goal, which otherwise would not have been possible because of their muscle problems on other statins. An estimated 1 to 2 million patients have ended statin therapy due to such side effects. The impression that prevalence of mild to moderate muscle-related side effects to statins is much higher in practice than in clinical trials was recently borne out in an observational study involving an unselected population of 7,924 French patients on high-dose statin therapy. The study — the Prediction of Muscular Risk in Observational conditions (PRIMO) as the first to look at statin-related side effects in clinical practice. It found that muscular symptoms occurred in 10.5% of patients. Thirty-eight percent of patients with muscle-related side effects said muscular pain prevented even moderate exertion during everyday activities.