Lovastatin is a cholesterol-lowering agent first isolated from a strain of Aspergillus terreus. It has been FDA-approved for the treatment and prevention of coronary heart disease, hypercholesterolemia, and adolescent patients with heterozygous familial hypercholesterolemia. Non-FDA approved uses include cardiac risk reduction for non-cardiac surgery and non-cardioembolic stroke.
Lovastatin is metabolized into its active form beta-hydroxy acid in the stomach and functions to competitively inhibit of 3-hydroxy-3-methylglutaryl-coenzyme A (HMG-CoA) reductase. This enzyme is involved in the rate-limiting step of cholesterol synthesis. HMG-CoA inhibitors also decrease levels of high-sensitivity C-reactive protein (hsCRP), improve endothelial function, reduce inflammation at coronary plaque sites, inhibit platelet aggregation, and has anticoagulant effects. Also, a decrease in serum cholesterol will stimulate LDL receptor expression on hepatocytes, further increasing LDL catabolism.
Lovastatin has a 30% bioavailability with an extensive first-pass effect; less than 5% reaches the systemic circulation. When administered without food, its bioavailability is reduced by 50%. It has a half-life of 1.1 to 1.7 hours, and greater than 95% protein binding. It is metabolized to beta-hydroxy acid (active form) by CYP3A4, with excretion of 80 to 85% in feces and 10% in urine. Therapeutic response is apparent by 2 weeks, and maximal response occurs within 4 to 6 weeks.
Lovastatin is available in two forms, immediate and extended-release tablets. Immediate-release tablets are recommended for administration in the evening with food, and extended-release taken at bedtime. Both dosage forms are not to be crushed or chewed.
Before starting Lovastatin, the patient should be started on a standard cholesterol-lowering diet for 6 weeks and continue this diet throughout treatment. Patients should avoid taking grapefruit juice since it may increase drug toxicity and adverse effects. Recommended starting dose is 20 mg once a day with an evening meal. The maximum recommended dose is 80mg in one day. Dosages should be individualized to treatment goal and adjusted at 4-week intervals.
Lovastatin immediate release is available in 20 mg and 40 mg tablets. The extended-release tablets are available in 20, 40, or 60 mg. Extended-release tablets are not recommended for patients that only need small amounts of reduction in cholesterol levels.
Lovastatin is generally well tolerated with mild and transient adverse reactions. There are few report cases of severe adverse effects associated with lovastatin. Below are the reported side effects of the drug:
Other serious adverse effects include diabetes mellitus, endocrine dysfunction, hepatotoxicity, and myopathy/rhabdomyolysis. Compared to other statins, lovastatin showed a non-significant upward trend in fasting blood glucose. Rarely reported was cognitive impairment (e.g., memory loss, forgetfulness, amnesia, memory impairment, confusion) which was non-serious and reversible. The FDA states that the cardiovascular benefits of statins outweigh the small risk of cognitive impairment.
Lovastatin use requires caution in older patients since they are predisposed to myopathy. Surgical patients should discontinue Lovastatin for elective major surgery, or any patients with conditions that may predispose them to renal failure (e.g., sepsis, hypotension, trauma, uncontrolled seizures). Lovastatin use in patients that have renal impairment and/or liver disease merits prescriber caution.
Lovastatin is contraindicated in patients with a history of hypersensitivity to lovastatin or any ingredient in its formulation. Other contraindications are listed below:
According to the American College of Cardiology and the American Heart Association Cholesterol Guideline Recommendations:
Lipid panel: baseline, fasting within 4 to 12 weeks after starting treatment or dose adjustment, and every 3 to 12 months after that. If 2 or more consecutive LDL levels are less than 40mg/dl, consider decreasing the dose.
Liver transaminase levels: baseline measure of hepatic transaminases. Measurement of the hepatic function of there is any indication of hepatotoxicity (e.g., unusual fatigue, loss of appetite, abdominal pain, dark-colored urine, jaundice, or scleral icterus) during therapy.
CPK: CPK levels do not require routine monitoring. Baseline CPK may be necessary for patients with a family history of statin intolerance, muscle disease, or taking other drugs that may increase the risk of myopathy. Any patients with muscle pain, weakness, aches or other symptoms suggestive of myopathy would need CPK levels.
Evaluate for new-onset diabetes: if diabetes develops, the patient is to continue statin therapy and encourage a healthy diet, exercise, maintaining healthy body weight, and cessation of tobacco use.
If the patient develops confusion or memory impairment, may evaluate for non-statin causes, systemic, or neuropsychiatric causes, and adverse effects associated with statin therapy.
Researchers gave a single 200 mg dose of lovastatin to 5 healthy volunteers, and there were no clinically significant adverse effects reported. There also have been cases of lovastatin overdose, but none of the patients reported any specific symptoms. All the patients recovered without complications.
The patient should discontinue lovastatin use if severe muscle symptoms or fatigue develops. CPK, creatinine, and urinalysis should be done to assess for myoglobinuria. Mild to moderate muscle symptoms should also call for discontinuation of lovastatin pending a thorough investigation of symptoms.
Lovastatin, like many other statin medications, is commonly used to help lower cholesterol levels. Although lovastatin shares several notable side effects with the other drugs in its class, it is generally well-tolerated. It could be beneficial for patients that are more sensitive to other statins. Lovastatin is effective in lowering cholesterol and the risk of atherosclerotic cardiovascular disease. Both patients and physicians should discuss the risks and benefits of lovastatin before starting treatment. Patients must also adhere to a heart-healthy diet before and during therapy with lovastatin. Patients should also know that routine checks are needed every 4 weeks to adjust and monitor serum levels of cholesterol.
Due to its many serious side effects and multiple drug-drug interactions, physicians, pharmacists, and patients must communicate with one another to provide optimal therapy. Pharmacists should notify both physicians and patients to discontinue any drugs that may cause harmful side effects while taking lovastatin. Nurses are well-positioned for monitoring adverse events related to the medication, as well as verifying medication compliance on the patient's part. It is important to establish strong communication between all disciplines of care to maximize the benefits of lovastatin; this includes interprofessional team communication between physicians (both primary care and/or cardiologist), nursing (particularly those with cardiovascular specialty training), and pharmacy to achieve optimal results from lovastatin therapy. [Level V]
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