National Lipid Association Scientific Statement on Statin Intolerance
- Authors:
- Cheeley MK, Saseen JJ, Agarwala A, et al.
- Citation:
- NLA Scientific Statement on Statin Intolerance: A New Definition and Key Considerations for ASCVD Risk Reduction in the Statin Intolerant Patient. J Clin Lipidol 2022;Jun 9:[Epub ahead of print].
The following are key points to remember about this scientific statement from the National Lipid Association (NLA) on statin intolerance:
- The purpose of this statement is to provide an updated definition of statin intolerance and to aid clinicians and researchers in identifying, managing, and investigating statin intolerance.
- Statin intolerance is defined as “one or more adverse effects associated with statin therapy, which resolves or improves with dose reduction or discontinuation, and can be classified as complete inability to tolerate any dose of a statin or partial intolerance, with inability to tolerate the dose necessary to achieve the patient-specific therapeutic objective. To classify a patient as having statin intolerance, a minimum of two statins should have been attempted, including at least one at the lowest approved daily dosage.”
- Incidence of statin intolerance (complete or partial) likely ranges from 5-30% and varies with the population studied.
- Statin intolerance may impact patient adherence. When patients demonstrate nonadherence or lack of persistence with statin therapy, clinicians should consider statin intolerance as a potential contributing factor.
- Adverse effects related to statins may include:
- Myalgias, which are the most common complaint, and may be described as muscle aches, pains, cramps, fatigue, or weakness; muscle-related complaints may be due in part to the "nocebo" effect, in which anticipation of harm results in the perception of side effects.
- Myopathy, which occurs in 1 out of 10,000 patients, and is characterized by unexplained muscle pain or weakness plus creatine kinase (CK) concentration >10 times the upper limit of normal.
- Rhabdomyolysis, which occurs in 1 out of 100,000 patients per year of therapy, and is characterized by creatine kinase (CK) typically >40 times the upper limit of normal; the elevated CK can cause myoglobinuria and acute renal failure; it is potentially life-threatening but usually reversible if detected early and treated appropriately.
- Elevation of transaminase levels, elevated blood glucose levels, and rarely, memory loss or confusion.
- Finding a statin regimen that is acceptable to the patient may require switching agents, trying a lower dosage, or use of alternative regimens such as on alternate days. Whenever possible, multiple attempts should be made to achieve statin tolerance, as most patients with reported statin intolerance can tolerate some degree of statin therapy. Complete statin intolerance is uncommon (<5% of patients).
- Statin-related adverse effects may be avoided or mitigated by correcting modifiable risk factor(s) for statin intolerance: hypothyroidism, alcohol use, strenuous exercise, vitamin D deficiency, obesity, diabetes, and drug interactions.
- Drugs known to potentially interact with statins include gemfibrozil, protease inhibitors, amiodarone, calcium channel blockers, azole antifungals, macrolides, immunosuppressants, and colchicine.
- If a patient is unable to reach therapeutic objective with lifestyle changes and maximally tolerated statin therapy, then nonstatin therapy may be needed. Nonstatin therapies that have demonstrated reduced adverse cardiovascular outcomes in randomized trials should be favored.
- In order to minimize the duration of exposure to high low-density lipoprotein levels, clinicians may consider initiating nonstatin therapy in high-risk and very-high-risk patients, while continuing attempts to identify a tolerable statin regimen.
Clinical Topics: Cardiovascular Care Team, Diabetes and Cardiometabolic Disease, Dyslipidemia, Prevention, Lipid Metabolism, Nonstatins, Novel Agents, Statins
Keywords: Amiodarone, Antifungal Agents, Atherosclerosis, Blood Glucose, Calcium Channel Blockers, Cardiometabolic Risk Factors, Colchicine, Creatine Kinase, Diabetes Mellitus, Dyslipidemias, Gemfibrozil, Hydroxymethylglutaryl-CoA Reductase Inhibitors, Hypothyroidism, Immunosuppressive Agents, Life Style, Lipoproteins, LDL, Medication Adherence, Muscle Cramp, Myalgia, Nocebo Effect, Obesity, Patient Care Team, Patient Compliance, Protease Inhibitors, Renal Insufficiency, Rhabdomyolysis, Risk Factors, Secondary Prevention, Transaminases, Vitamin D Deficiency
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