Statin-Associated Muscle Symptoms: Impact On Statin Therapy-European Atherosclerosis Society Consensus Panel Statement On Assessment, Aetiology And Management
Tarih
2015Yazar
Stroes, Erik S.
Thompson, Paul D.
Corsini, Alberto
Vladutiu, Georgirene D.
Raal, Frederick J.
Ray, Kausik K.
Roden, Michael
Stein, Evan
Tokgozoglu, Lale
Nordestgaard, Borge G.
Bruckert, Eric
De Backer, Guy
Krauss, Ronald M.
Laufs, Ulrich
Santos, Raul D.
Hegele, Robert A.
Hovingh, G. Kees
Leiter, Lawrence A.
Mach, Francois
Maerz, Winfried
Newman, Connie B.
Wiklund, Olov
Jacobson, Terry A.
Catapano, Alberico L.
Chapman, M. John
Ginsberg, Henry N.
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Statin-associated muscle symptoms (SAMS) are one of the principal reasons for statin non-adherence and/or discontinuation, contributing to adverse cardiovascular outcomes. This European Atherosclerosis Society (EAS) Consensus Panel overviews current understanding of the pathophysiology of statin-associated myopathy, and provides guidance for diagnosis and management of SAMS. Statin-associated myopathy, with significant elevation of serum creatine kinase (CK), is a rare but serious side effect of statins, affecting 1 per 1000 to 1 per 10 000 people on standard statin doses. Statin-associated muscle symptoms cover a broader range of clinical presentations, usually with normal or minimally elevated CK levels, with a prevalence of 7-29% in registries and observational studies. Preclinical studies show that statins decrease mitochondrial function, attenuate energy production, and alter muscle protein degradation, thereby providing a potential link between statins and muscle symptoms; controlled mechanistic and genetic studies in humans are necessary to further understanding. The Panel proposes to identify SAMS by symptoms typical of statin myalgia (i.e. muscle pain or aching) and their temporal association with discontinuation and response to repetitive statin rechallenge. In people with SAMS, the Panel recommends the use of a maximally tolerated statin dose combined with non-statin lipid-lowering therapies to attain recommended low-density lipoprotein cholesterol targets. The Panel recommends a structured work-up to identify individuals with clinically relevant SAMS generally to at least three different statins, so that they can be offered therapeutic regimens to satisfactorily address their cardiovascular risk. Further research into the underlying pathophysiological mechanisms may offer future therapeutic potential.