Simvastatin: Comprehensive Drug Monograph

Quick Facts

Pharmacokinetic Profile

Half-Life

~2 h (parent); ~2–4 h (active acid)

Metabolism

Extensive CYP3A4 / CYP3A5

Protein Binding

~95%

Bioavailability

<5% (extensive first-pass metabolism)

Active Form

Lactone prodrug → simvastatin acid

Clinical Information

Drug Class

HMG-CoA reductase inhibitor

Available Strengths

Zocor 10, 20, 40 mg tablets; generic also at 5 mg; 80 mg restricted; FloLipid suspension 20 mg/5 mL and 40 mg/5 mL

Route & Timing

Oral, once daily in the evening

Maximum Recommended

40 mg/day (80 mg restricted use)

Renal Adjustment

Severe CKD (CrCl <30): start 5 mg/day

Hepatic Status

Caution in chronic alcohol use or prior liver disease

Pregnancy

Not contraindicated since FDA July 2021 update; usually discontinued

Lactation

Not recommended

Schedule / Status

Rx only; not a controlled substance

Generic Available

Yes (since June 2006); brand Zocor approved 1991

Indications

Indication	Approved Population	Therapy Type	Status
Reduction of total mortality, CHD death, non-fatal MI, stroke, and need for revascularization	Adults with established CHD, cerebrovascular disease, peripheral vascular disease, and/or diabetes who are at high risk of CHD events	Adjunct to diet	FDA Approved
Primary hyperlipidemia	Adults	Adjunct to diet	FDA Approved
Heterozygous familial hypercholesterolemia (HeFH)	Adults and pediatric patients aged 10 years and older	Adjunct to diet	FDA Approved
Homozygous familial hypercholesterolemia (HoFH)	Adults	Adjunct to other LDL-C-lowering therapies (e.g., LDL apheresis, ezetimibe)	FDA Approved
Hypertriglyceridemia (Fredrickson type IV)	Adults	Adjunct to diet	FDA Approved
Primary dysbetalipoproteinemia (Fredrickson type III)	Adults	Adjunct to diet	FDA Approved

Simvastatin was the first statin to demonstrate a mortality benefit in a large outcome trial — the 1994 Scandinavian Simvastatin Survival Study (4S) showed a 30% reduction in all-cause mortality and 42% reduction in CHD mortality in patients with established CHD over a median 5.4 years. The Heart Protection Study (HPS) subsequently confirmed cardiovascular benefit across a broader high-risk population (diabetes, peripheral vascular disease, prior stroke) regardless of baseline LDL-C, with a 13% reduction in all-cause mortality and 18% reduction in vascular mortality. The 2018 AHA/ACC Cholesterol Guideline classifies simvastatin 20–40 mg as moderate intensity (LDL-C reduction ~30–49%) and simvastatin 10 mg as low intensity (<30%); no simvastatin dose meets the high-intensity threshold (≥50%) — even 80 mg achieves only ~46% LDL-C reduction in the VOYAGER meta-analysis, and 80 mg is no longer recommended for new initiation due to myopathy risk.

Off-Label Uses

Stroke prevention beyond approved indications — extrapolation from class-wide CTT meta-analyses for patients with high ASCVD risk. Evidence: high quality (extrapolated).

Diabetic dyslipidemia in primary prevention — used as a moderate-intensity option, particularly when cost is a concern; HPS supports benefit. Evidence: moderate quality.

Aortic valve calcification slowing — investigated in SEAS and other trials; the data have not supported a meaningful effect on disease progression. Evidence: low quality (negative trials).

Dose

Dosing

All doses are administered orally, once daily, in the evening (cholesterol biosynthesis peaks overnight, so evening dosing maximizes pharmacodynamic effect for short-half-life statins). Reassess LDL-C as early as 4 weeks after initiation or dose change. The maximum recommended dosage is 40 mg/day; the 80 mg dose is restricted to patients who have already tolerated it chronically (≥12 months) without muscle toxicity and is not appropriate for new initiation or up-titration. Note that simvastatin 10 mg is classified as low-intensity therapy by the 2018 AHA/ACC guideline; only 20 mg or higher meets the moderate-intensity threshold.

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Primary hyperlipidemia — moderate-intensity goal (LDL-C reduction 30–49%)	20 mg evening	20–40 mg evening	40 mg/day	20–40 mg = moderate intensity per AHA/ACC 2018 Per VOYAGER meta-analysis: ~32% LDL-C reduction at 20 mg, ~37% at 40 mg. 10 mg is low intensity (~28% reduction)
ASCVD secondary prevention (post-MI, post-stroke, established CAD/PAD, diabetes with high CHD risk)	40 mg evening	40 mg evening	40 mg/day	If <50% LDL-C reduction goal not met at 40 mg, switch to a high-intensity statin (atorvastatin 40–80 or rosuvastatin 20–40) rather than escalate to 80 mg HPS evidence supports 40 mg in this population
Heterozygous familial hypercholesterolemia (HeFH) — adults	20–40 mg evening	40 mg evening	40 mg/day	If goal not achieved, add ezetimibe or a PCSK9 inhibitor rather than escalate dose
Heterozygous familial hypercholesterolemia (HeFH) — pediatric ≥10 years	10 mg evening	10–40 mg evening	40 mg/day	Adjust at intervals of ≥4 weeks. Doses >40 mg not studied in this population Adolescent females: counsel on contraception
Homozygous familial hypercholesterolemia (HoFH)	40 mg evening	40 mg evening (80 mg permitted in patients chronically tolerating it without muscle toxicity)	80 mg/day (restricted use)	Use as adjunct to other LDL-C-lowering therapy (LDL apheresis, ezetimibe, PCSK9 inhibitor, lomitapide) Per FDA label HoFH study (n=12): mean LDL-C reduction 30% (range 14–46%) at 80 mg/day; 14% at 40 mg/day
Hypertriglyceridemia / primary dysbetalipoproteinemia	20 mg evening	20–40 mg evening	40 mg/day	Modest TG reduction (~20–30%); consider fenofibrate or icosapent ethyl if TG remain elevated Gemfibrozil is contraindicated
Continuation of pre-existing 80 mg dose (legacy patients only)	Not for new initiation	80 mg evening (only if tolerated ≥12 months without muscle toxicity)	80 mg/day	Do NOT initiate 80 mg in new patients. Switch to alternate statin if any new interacting drug is started or if myopathy risk emerges FDA restricted 80 mg in 2011 due to myopathy data from SEARCH

Population-Specific Adjustments

Population	Starting / Recommended Dose	Maximum Dose	Notes
Severe renal impairment (CrCl <30 mL/min/1.73 m²)	5 mg evening (use 5 mg generic; Zocor 5 mg no longer marketed)	Cautious titration; close monitoring	Higher plasma concentrations and elevated myopathy risk
Chinese ancestry on lipid-modifying niacin (≥1 g/day)	Limit to 20 mg evening	20 mg/day with niacin	Increased myopathy risk observed in HPS2-THRIVE; do not use 80 mg with niacin in this population
Concomitant verapamil, diltiazem, or dronedarone	Standard initiation	10 mg/day	CYP3A4 inhibition raises myopathy risk substantially
Concomitant amiodarone, amlodipine, or ranolazine	Standard initiation	20 mg/day	Moderate CYP3A4 inhibition; the dose cap was retained after the 2011 FDA review
Concomitant lomitapide (HoFH)	Reduce existing dose by 50%	20 mg/day (or 40 mg if previously chronic 80 mg)	Lomitapide approximately doubles simvastatin exposure
Concomitant ticagrelor	Standard initiation	40 mg/day	Ticagrelor inhibits CYP3A4; do not use higher doses
Mild–moderate hepatic impairment	Use cautiously; standard initiation	Standard maxima	Acute liver failure or decompensated cirrhosis warrants alternative therapy
Elderly (≥65 years)	Lower starting dose (10 mg) reasonable	Standard maxima	Risk factor for myopathy per the PI; 4S and HPS showed similar efficacy and safety

Clinical Pearl — Why Evening Dosing

Simvastatin has a short half-life (~2 hours) and the active acid metabolite has a similarly short half-life (~2–4 hours). Endogenous cholesterol synthesis is highest during the night, so evening administration synchronises peak drug effect with peak HMG-CoA reductase activity and produces meaningfully greater LDL-C reduction than morning dosing. This timing rule applies to all short-acting statins (lovastatin, simvastatin) and not to long-acting statins (atorvastatin, rosuvastatin), which can be taken any time.

Clinical Pearl — Don’t Up-Titrate to 80 mg

If a patient is not at LDL-C goal on simvastatin 40 mg, the correct move is to switch to a higher-intensity statin (atorvastatin 40–80 mg or rosuvastatin 20–40 mg) or add ezetimibe — not to escalate to simvastatin 80 mg. The 80 mg dose carries roughly 8-fold higher myopathy risk than the 40 mg dose and is reserved for patients already tolerating it long-term. Patients on 80 mg who need to start an interacting drug should be switched to a different statin rather than have the interacting drug added.

Pharmacology

Mechanism of Action

Simvastatin is administered as an inactive lipophilic lactone prodrug that is hydrolysed in the liver — primarily by carboxylesterases and paraoxonases — to its active β-hydroxyacid form, simvastatin acid. The active acid is a competitive, reversible inhibitor of 3-hydroxy-3-methylglutaryl coenzyme A (HMG-CoA) reductase, the rate-limiting enzyme converting HMG-CoA to mevalonate in hepatic cholesterol biosynthesis. Reduced intracellular cholesterol upregulates LDL receptors on hepatocyte surfaces, increasing clearance of LDL particles from circulation. Net effects are dose-dependent reductions in LDL-C (approximately 28–46% across the 10–80 mg dose range per the VOYAGER meta-analysis), apolipoprotein B, non-HDL-C, and total cholesterol, with smaller reductions in triglycerides (~10–30%) and modest increases in HDL-C (~5–15%).

Because simvastatin is a lipophilic statin with extensive first-pass metabolism, it is more vulnerable to CYP3A4-driven drug interactions than the hydrophilic statins (pravastatin, rosuvastatin). Inhibitors of CYP3A4 — strong (azole antifungals, macrolide antibiotics, certain HIV antiretrovirals, cobicistat, nefazodone) or moderate (verapamil, diltiazem, amiodarone, amlodipine, ranolazine, dronedarone, ticagrelor) — substantially raise simvastatin exposure and predictably raise myopathy risk. Simvastatin acid is a substrate of OATP1B1 (encoded by SLCO1B1), which adds a second mechanism for interactions with cyclosporine, gemfibrozil, and similar transporter inhibitors; the SEARCH GWAS identified SLCO1B1 variants as the dominant genetic determinant of simvastatin-induced myopathy.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Tmax ~1.8 h (parent), ~4.2 h (acid); absolute bioavailability <5%; food has minimal effect	Take in the evening; food does not require dose adjustment
Distribution	Plasma protein binding ~95%; lipophilic — distributes broadly into tissues including muscle	Greater extrahepatic exposure than hydrophilic statins; contributes to higher myopathy risk profile at high doses
Metabolism	Extensive CYP3A4 (and CYP3A5) metabolism in intestine and liver; active metabolites including 6′-hydroxy, 6′-hydroxymethyl, and 6′-exomethylene simvastatin acid	The dominant source of clinically important drug interactions; grapefruit juice (intestinal CYP3A4 inhibitor) significantly elevates exposure
Elimination	~60% excreted in feces, ~13% in urine (mostly as metabolites); t½ short (~2 h parent, ~2–4 h acid)	Short half-life is the basis for evening dosing; severe renal impairment requires dose reduction

Side Effects

Adverse-effect frequencies below are from the simvastatin controlled clinical trials database (n = 2,423, median follow-up 18 months) and the major outcome trials (4S, HPS, SEARCH), as reported in the current FDA Zocor prescribing information. Real-world rates of muscle and gastrointestinal symptoms are typically higher than pivotal-trial reports because of selection criteria and the well-described nocebo effect.

≥10% Very Common

No adverse reaction crossed the 10% threshold in the FDA Zocor pre-marketing clinical-trial database. Pooled observational data place statin-associated muscle symptoms in the 5–10% range, but these signals are not represented in the placebo-controlled labelling tables. The most common reactions (≥5%) are listed in the next tier.

1–10% Common

Adverse Effect	Incidence	Clinical Note
Upper respiratory tract infection	9%	Likely background population rate rather than drug-attributable
Headache	7%	Generally mild; usually resolves within weeks
Abdominal pain	7%	Usually mild; rule out gallbladder disease if severe or worsening
Constipation	7%	Typically responsive to fiber and hydration
Nausea	5%	Usually transient; take in evening with light snack if bothersome
Asymptomatic ALT/AST elevation >3× ULN (persistent)	~0.9% at 40 mg; ~2.1% at 80 mg	Reversible on discontinuation; not predictive of clinical hepatotoxicity
Asymptomatic CK elevation ≥3× ULN	~5%	Most attributable to non-cardiac CK fraction; not by itself an indication to stop
New-onset diabetes mellitus (statin class effect)	~1–2% excess risk	Concentrated in patients with prediabetes / metabolic syndrome; CV benefit substantially outweighs glycemic risk

Other adverse reactions reported in clinical trials: diarrhea, rash, dyspepsia, flatulence, asthenia, myalgia (each at lower frequency than the items above).

Serious Serious Adverse Effects

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Myopathy (CK >10× ULN with symptoms) — clinical trial database (24,747 patients, median 4 years)	~0.03% (20 mg) · ~0.08% (40 mg) · ~0.61% (80 mg)	Highest in first year; then declines	Discontinue; rechallenge with lower dose or alternate statin only after resolution
Myopathy in SEARCH (12,064 post-MI patients, mean 6.7 years)	~0.02% (20 mg) · ~0.9% (80 mg)	First year	Underlies the FDA 2011 restriction on the 80 mg dose
Rhabdomyolysis (CK >40× ULN) — SEARCH	~0% (20 mg) · ~0.4% (80 mg)	Weeks–months	Stop drug immediately; check CK and renal function; aggressive hydration; avoid all statins until resolved
Immune-mediated necrotizing myopathy (IMNM)	Very rare (~2 per million person-years across statin class)	Months–years; persists or worsens after stopping	Permanent discontinuation; check anti-HMGCR antibody; refer to neurology / rheumatology for immunosuppressive therapy
Fatal and non-fatal hepatic failure	Rare (post-marketing)	Weeks–months	Discontinue if jaundice or hyperbilirubinemia; evaluate for other causes
Hypersensitivity (anaphylaxis, angioedema, Stevens-Johnson syndrome, DRESS)	Rare (post-marketing)	Days–weeks	Permanent discontinuation; avoid all statins after anaphylaxis or severe cutaneous reaction
Cognitive impairment (memory loss, confusion — usually reversible)	Rare (post-marketing, statin class label)	Days to years; resolution typically within weeks of stopping	Trial of discontinuation if temporally related; not a contraindication to future statin therapy
Interstitial lung disease, peripheral neuropathy, thrombocytopenia, pancreatitis, polymyositis / dermatomyositis (statin class)	Very rare (post-marketing)	Months–years	Discontinue if temporally related and other causes excluded

Discontinuation Discontinuation Rates

Pre-marketing controlled trials (median 18 months)

1.4%

Top reasons: gastrointestinal disorders 0.5%, myalgia 0.1%, arthralgia 0.1%

Heart Protection Study (HPS, 40 mg, 5 years)

4.8% vs 5.1% placebo

Notable: discontinuation rates were similar to placebo over 5 years in 20,536 high-risk patients

Reason for Discontinuation	Context	Comment
Gastrointestinal disorders	0.5% in pre-marketing trials	Most common reason; usually settles or improves with food / evening dosing
Myalgia	0.1% in pre-marketing trials	Real-world rate is meaningfully higher; remains the most common open-label reason for discontinuation
Arthralgia	0.1% in pre-marketing trials	Often resolves after a few weeks
Hepatic enzyme elevation	~0.9% (40 mg) to ~2.1% (80 mg) develop persistent ALT/AST >3× ULN; not all discontinue	Many cases resolve on dose reduction; rarely indicative of clinical hepatotoxicity
Hypersensitivity	Permanent discontinuation indicated	Switch class if needed

Pediatric data (24-week controlled trial in 175 HeFH patients ages 10–17, with 144 in 24-week extension): adverse-reaction profile was similar to placebo; the most common adverse reactions were upper respiratory infection, headache, abdominal pain, and nausea. No detectable effect on growth or sexual maturation; doses >40 mg/day not studied in this population.

Managing Statin-Associated Muscle Symptoms (SAMS) — Simvastatin-Specific Considerations

For simvastatin specifically, drug-interaction-related myopathy is the dominant risk: a careful medication review (CYP3A4 inhibitors, including grapefruit juice ≥1 quart/day) often identifies a reversible cause. Stepwise approach: (1) confirm symptoms with a 4–6 week drug holiday; (2) check TSH, vitamin D, and creatinine; (3) review for new CYP3A4 inhibitors or interacting drugs; (4) if true SAMS confirmed, consider switching to a hydrophilic statin (rosuvastatin or pravastatin), which is less prone to CYP3A4-driven myotoxicity; (5) if statin truly intolerated, escalate to ezetimibe ± PCSK9 inhibitor or bempedoic acid.

Int

Drug Interactions

Simvastatin’s interaction profile is dominated by CYP3A4 inhibition. Strong CYP3A4 inhibitors are contraindicated; moderate CYP3A4 inhibitors require specific dose caps. Simvastatin acid is also a substrate of OATP1B1, accounting for the contraindications with cyclosporine and gemfibrozil. Always review the full medication list — including prescription, OTC, herbal (St. John’s wort), and dietary (grapefruit juice) — before initiating, escalating, or refilling simvastatin.

Contraindicated Strong CYP3A4 inhibitors — azole antifungals (itraconazole, ketoconazole, posaconazole, voriconazole)

MechanismProfound CYP3A4 inhibition; simvastatin AUC may rise 10- to 20-fold

EffectMarkedly increased risk of rhabdomyolysis

ManagementSuspend simvastatin during the antifungal course; restart afterward. Use fluconazole at lower doses with caution; consider pravastatin or rosuvastatin for transplant or chronic-antifungal patients

FDA PI

Contraindicated Macrolide antibiotics — erythromycin, clarithromycin, telithromycin

MechanismStrong CYP3A4 inhibition

EffectSeveral-fold rise in simvastatin exposure with documented rhabdomyolysis

ManagementSuspend simvastatin during the antibiotic course. Azithromycin is an acceptable alternative with no clinically significant CYP3A4 inhibition

FDA PI

Contraindicated HIV / HCV protease inhibitors and cobicistat-containing products (e.g., ritonavir, nelfinavir, darunavir/ritonavir, atazanavir/cobicistat, elvitegravir/cobicistat)

MechanismPotent CYP3A4 inhibition

EffectMajor rises in simvastatin exposure; documented rhabdomyolysis

ManagementAvoid combination. Pravastatin or pitavastatin are preferred statins in HIV-infected patients; rosuvastatin is acceptable at reduced dose

FDA PI

Contraindicated Nefazodone, boceprevir, telaprevir

MechanismStrong CYP3A4 inhibition

EffectMultifold rise in simvastatin levels

ManagementAvoid combination; suspend simvastatin during therapy

FDA PI

Contraindicated Cyclosporine

MechanismCYP3A4 and OATP1B1 inhibition

EffectSeveral-fold rise in simvastatin acid exposure; markedly elevated rhabdomyolysis risk

ManagementCombination contraindicated. Use pravastatin (no transporter affinity issues) or fluvastatin in transplant patients

FDA PI

Contraindicated Gemfibrozil

MechanismOATP1B1 and glucuronidation interference; additive intrinsic muscle toxicity

Effect~3-fold rise in simvastatin acid AUC; substantial rhabdomyolysis risk

ManagementCombination contraindicated. Fenofibrate is an acceptable alternative when a fibrate is required

FDA PI

Contraindicated Danazol

MechanismCYP3A4 inhibition and additive myotoxicity

EffectIncreased rhabdomyolysis risk reported in case series

ManagementCombination contraindicated

FDA PI

Major Verapamil, diltiazem, dronedarone

MechanismModerate CYP3A4 inhibition; verapamil also inhibits P-glycoprotein

Effect~2- to 5-fold rise in simvastatin exposure; increased myopathy

ManagementDo not exceed simvastatin 10 mg/day

FDA PI

Major Amiodarone, amlodipine, ranolazine

MechanismModerate CYP3A4 inhibition

EffectModest rise in simvastatin exposure with associated myopathy reports

ManagementDo not exceed simvastatin 20 mg/day

FDA PI

Major Lomitapide

MechanismCYP3A4-mediated interaction

EffectApproximately doubles simvastatin exposure

ManagementReduce existing simvastatin dose by 50%; do not exceed 20 mg/day (or 40 mg if patient was previously chronic on 80 mg without toxicity)

FDA PI

Major Ticagrelor

MechanismCYP3A4 inhibition

EffectModest rise in simvastatin exposure

ManagementDo not exceed simvastatin 40 mg/day

Lexicomp · Ticagrelor PI

Major Grapefruit juice (large quantities, >1 quart/day)

MechanismIrreversible inhibition of intestinal CYP3A4 by furanocoumarins

EffectSeveral-fold rise in simvastatin AUC; documented myopathy

ManagementAvoid large amounts. Modest, occasional consumption (small glasses) is generally acceptable

FDA PI

Moderate Niacin (lipid-modifying ≥1 g/day)

MechanismAdditive skeletal muscle toxicity (no clinically meaningful PK interaction)

EffectIncreased risk of myopathy, particularly in Chinese patients; HPS2-THRIVE showed no CV benefit

ManagementRoutine combination not recommended. In Chinese patients, do not exceed simvastatin 20 mg/day with niacin and avoid 80 mg combination outright

FDA PI

Moderate Fenofibrate

MechanismAdditive muscle and renal effects (independent of OATP1B1)

EffectModest myopathy risk; combination broadly safer than gemfibrozil

ManagementAcceptable when both agents are clinically indicated; counsel on muscle symptoms

FDA PI

Moderate Colchicine

MechanismAdditive myotoxicity

EffectIncreased risk of myopathy / rhabdomyolysis, especially with chronic use or renal impairment

ManagementUse lowest effective colchicine dose; counsel on muscle symptoms; check CK if symptoms develop

FDA PI · Case reports

Moderate Daptomycin

MechanismAdditive skeletal muscle toxicity

EffectIncreased risk of myopathy / rhabdomyolysis

ManagementTemporarily suspend simvastatin during the daptomycin course

FDA PI

Moderate Coumarin anticoagulants (warfarin)

MechanismMechanism unclear; possible CYP-mediated effect

EffectModest INR prolongation

ManagementAchieve a stable INR before starting simvastatin; monitor INR more closely on initiation, dose change, or discontinuation

FDA PI

Moderate Digoxin

MechanismModest effect on digoxin pharmacokinetics

EffectSlight elevation in digoxin levels (~0.3 ng/mL increase reported in PI)

ManagementNo routine dose adjustment required; standard digoxin monitoring

FDA PI

Minor St. John’s Wort

MechanismCYP3A4 induction

EffectDecreased simvastatin exposure; reduced LDL-C lowering effect

ManagementCounsel patients to avoid; document on the medication review

Pharmacokinetic studies

Minor Bile acid sequestrants (cholestyramine, colestipol)

MechanismReduced absorption

EffectModest decrease in simvastatin levels

ManagementTake simvastatin at least 2 hours before or 4 hours after the sequestrant

FDA PI

Mon

Monitoring

Lipid Panel Baseline; reassess as early as 4 weeks; then 4–12 weeks after dose change; then annually
Routine Confirm percent LDL-C reduction (~32% expected at 20 mg, ~37% at 40 mg per VOYAGER). If <50% reduction is needed, switch to a higher-intensity statin rather than escalate simvastatin to 80 mg. Adherence is a more common reason for inadequate response than non-response.
ALT / AST Baseline; thereafter only if symptoms
Trigger-based Routine periodic LFTs are no longer recommended. Repeat if patient develops jaundice, fatigue, abdominal pain, dark urine, or unexplained nausea. Discontinue if ALT/AST >3× ULN with symptoms or hyperbilirubinemia.
Creatine Kinase (CK) Baseline only in high-risk patients; otherwise only if symptoms
Trigger-based High-risk = age ≥65, hypothyroidism, renal impairment, prior statin myopathy, Chinese ancestry on niacin, or concomitant CYP3A4 inhibitor. Check if patient develops myalgia, weakness, or dark urine. Stop if CK >10× ULN with symptoms.
Medication Reconciliation Every visit and at every new prescription
Routine Specifically check for new CYP3A4 inhibitors (especially azole antifungals, clarithromycin, ritonavir-containing antiretrovirals, cobicistat, calcium channel blockers, amiodarone) and grapefruit juice intake. Adjust dose or switch agents proactively.
HbA1c / Fasting Glucose Baseline; periodically if at risk for diabetes
Routine Modest excess incidence of new-onset diabetes (mostly in patients with prediabetes). CV benefit greatly outweighs glycemic risk; do not stop the statin if A1c rises into diabetic range.
Renal Function Baseline; per overall comorbidity profile
Routine Estimate CrCl/eGFR before initiation and recheck if clinical change. Severe CKD (CrCl <30 mL/min/1.73 m²) requires starting at 5 mg.
TSH If unexplained myalgia or rising CK
Trigger-based Unrecognized hypothyroidism is a major contributor to apparent statin intolerance and CK rise; treat the thyroid before declaring statin intolerance.
Adherence Check Every clinical visit
Routine Approximately half of patients discontinue statins within 1 year of initiation. Open, non-judgemental questioning (“How often do you forget?”) yields more accurate information than yes/no adherence questions. Confirm patient is taking the dose in the evening.
Pregnancy Status In females of reproductive potential, periodically
Trigger-based FDA removed the pregnancy contraindication in July 2021. Statins are generally discontinued during planned or confirmed pregnancy unless benefits clearly outweigh risk (e.g., HoFH or established ASCVD). Effective contraception is recommended during therapy.

Contraindications & Cautions

Absolute Contraindications (per current FDA Zocor PI, Organon 2023)

Concomitant use of strong CYP3A4 inhibitors — including itraconazole, ketoconazole, posaconazole, voriconazole, erythromycin, clarithromycin, telithromycin, HIV protease inhibitors (e.g., ritonavir, nelfinavir, darunavir/ritonavir), boceprevir, telaprevir, nefazodone, and cobicistat-containing products.
Concomitant cyclosporine, danazol, or gemfibrozil.
Hypersensitivity to simvastatin or any formulation excipient (anaphylaxis, angioedema, and Stevens-Johnson syndrome have been reported).

Note on label discrepancy: The FloLipid (oral suspension) prescribing information additionally lists “active liver disease, which may include unexplained persistent elevations in hepatic transaminase levels” as a contraindication. The current Zocor (tablet) PI does not include this in its Contraindications section but addresses hepatic dysfunction under Warnings and Precautions. Clinicians prescribing the suspension formulation should follow the FloLipid label.

Relative Contraindications (Specialist Input Recommended)

Acute liver failure or decompensated cirrhosis — although not listed in the Zocor PI Contraindications section, statins are generally avoided. The Zocor PI states use with caution in chronic alcohol use or prior liver disease and lists hepatic dysfunction as a Warning.
Pregnancy — although the FDA removed the contraindication in 2021, statins are still typically discontinued during planned or confirmed pregnancy. Continued use is reasonable only in HoFH or established ASCVD where lipid-lowering benefit clearly outweighs theoretical fetal risk; document the explicit risk-benefit discussion. For most patients, switching to a hydrophilic statin (rosuvastatin, pravastatin) or stopping is preferred.
Lactation — breastfeeding is not recommended during simvastatin therapy; if therapy is required postpartum, use formula.
Severe renal impairment (CrCl <30 mL/min/1.73 m²) — start at 5 mg/day with close monitoring.
History of statin-induced rhabdomyolysis or immune-mediated necrotizing myopathy — IMNM is a permanent contraindication to all statins; uncomplicated SAMS may permit cautious rechallenge with a different statin.
Currently tolerating 80 mg with new interacting drug — switch to an alternate statin rather than continuing 80 mg with the interacting agent.

Use with Caution

Chinese ancestry on lipid-modifying niacin — do not exceed 20 mg simvastatin with niacin ≥1 g/day; avoid the 80 mg dose with niacin in this group entirely.
Age ≥65 years — frailty, polypharmacy, and lower muscle mass raise myopathy risk; start at 10 mg.
Hypothyroidism — treat first; untreated hypothyroidism amplifies myopathy risk and may itself elevate CK.
Concomitant fibrates (especially fenofibrate), niacin (≥1 g/day), colchicine, or daptomycin — additive myotoxicity; counsel on muscle symptoms and consider temporarily suspending simvastatin during a daptomycin course.
Diabetes risk factors (prediabetes, metabolic syndrome) — small excess diabetes incidence; CV benefit nonetheless outweighs risk.
Major surgery, sepsis, severe trauma, or other acute serious medical conditions — temporarily withhold simvastatin in any patient at high risk of rhabdomyolysis.
Pediatric patients <10 years — efficacy and safety not established below age 10.
Myasthenia gravis or ocular myasthenia — case reports of new onset or worsening with statin use; weigh carefully.

FDA Drug Safety Communication (June 2011) Restriction on the 80 mg Dose of Simvastatin

The FDA restricted use of the simvastatin 80 mg dose because of an increased risk of muscle injury, particularly during the first year of therapy. Simvastatin 80 mg should not be initiated in new patients. The 80 mg dose is reserved only for patients who have been taking it chronically (≥12 months) without evidence of muscle toxicity. For patients on 40 mg who are not at LDL-C goal, prescribe an alternative LDL-C-lowering treatment (different statin or addition of ezetimibe or PCSK9 inhibitor) rather than escalating to 80 mg. Patients tolerating 80 mg who are starting an interacting drug must be switched to an alternate statin.

Risk basis: in the SEARCH trial (12,064 post-MI patients, 6.7 years), myopathy occurred in approximately 0.9% on 80 mg vs 0.02% on 20 mg, with rhabdomyolysis in 0.4% vs 0%.

FDA Class-Wide Regulatory Update Statin Use During Pregnancy — FDA Communication of July 20, 2021

The FDA requested removal of the contraindication against statin use in pregnancy from the labeling of all statins. The change does not endorse routine use; it allows individualized risk-benefit decisions, particularly for women with HoFH, established ASCVD, or very high CV risk.

Most patients should still discontinue statins on confirmation of pregnancy. Lactation remains a reason to defer therapy because of potential infant exposure; patients who require ongoing statin therapy postpartum should not breastfeed.

FDA Class-Wide Regulatory Warning Myopathy and Rhabdomyolysis — Heightened Risk for Simvastatin

All HMG-CoA reductase inhibitors carry a class-wide warning regarding myopathy and rhabdomyolysis. Simvastatin’s CYP3A4-driven metabolism makes it particularly susceptible to dose-dependent and interaction-driven myopathy. Risk factors include age ≥65 years, uncontrolled hypothyroidism, renal impairment, female sex, low body weight, Chinese ancestry, and concomitant interacting drugs.

Counsel every patient to promptly report unexplained muscle pain, tenderness, weakness, or dark urine. Discontinue immediately if rhabdomyolysis is suspected or if CK rises >10× ULN with symptoms. Temporarily withhold simvastatin in any patient with an acute serious condition predisposing to rhabdomyolysis (sepsis, hypotension, dehydration, major surgery, severe metabolic or electrolyte disorder, uncontrolled seizures).

Patient Counselling

Purpose of Therapy

Simvastatin lowers LDL (“bad”) cholesterol by reducing the liver’s production of cholesterol. Lower LDL means less plaque buildup inside arteries, which reduces the chance of heart attacks, strokes, and the need for procedures such as stents or bypass surgery. The benefit accumulates over years — most patients are taking it for prevention rather than for symptom relief, so they may not “feel” anything different. Lifestyle measures (diet, exercise, weight control, smoking cessation) act on the same arteries and add to the benefit.

How to Take

Take one tablet once a day, in the evening, with or without food. Evening dosing matters for this medicine specifically — the body makes most of its cholesterol overnight, so an evening dose works better than a morning dose. If a dose is missed, take it as soon as remembered the same evening; if the next dose is due within a few hours, skip the missed one and continue normally. Do not double up. Avoid drinking large amounts of grapefruit juice (more than about a quart per day); occasional small servings are fine. Do not stop the medicine without speaking to the prescriber, even if cholesterol numbers look good — stopping is when the protection fades.

Muscle Pain or Weakness

Tell patient Some mild aches in the first few weeks are common and often unrelated to the medicine. They usually settle. Stay hydrated, especially during exercise. Severe weakness or pain that affects walking or stair-climbing is not normal. Risk goes up at higher doses (especially 80 mg) and when other medicines are added.

Call prescriber Severe or persistent muscle pain, unexplained weakness, fatigue out of proportion to activity, or dark / cola-colored urine. Seek same-day care for the dark-urine combination.

Other Medicines, Including Over-the-Counter and Herbal

Tell patient Always tell every healthcare provider — including dentists and pharmacists — that simvastatin is on the list. Several common medicines do not mix safely with simvastatin: certain antibiotics (clarithromycin, erythromycin), certain antifungals (-azole names ending in “-conazole”), HIV and hepatitis C medicines, cyclosporine after transplant, gemfibrozil, danazol, and several heart medicines (verapamil, diltiazem, amiodarone, amlodipine). Avoid St. John’s Wort, which lowers the medicine’s effect.

Call prescriber Before starting any new prescription, especially antibiotics, antifungals, HIV / hepatitis medications, or new heart medications. Simvastatin may need to be paused or switched.

Grapefruit and Grapefruit Juice

Tell patient Large amounts of grapefruit juice (more than about a quart per day) can make this medicine build up to dangerous levels in the body. A small glass occasionally is generally safe; daily large servings are not. If grapefruit is a regular part of the diet, discuss switching to a different statin that is not affected by grapefruit (such as rosuvastatin or pravastatin).

Call prescriber If unsure about grapefruit intake; if muscle pain develops after grapefruit use.

“I Feel Fine — Why Am I Taking This?”

Tell patient High cholesterol does not cause symptoms. The medication’s job is to prevent a future heart attack or stroke, not to make today feel different. Stopping it because nothing feels different is the most common cause of preventable cardiovascular events in clinic populations.

Call prescriber Before stopping or skipping doses for any reason. New side effects, planned pregnancy, planned surgery, or any new prescription from another clinician.

Pregnancy Plans

Tell patient If pregnancy is being planned, the prescriber will usually pause the statin before conception. If pregnancy is discovered while taking it, contact the clinic — do not panic. Recent FDA review of cohort data did not show a clear pattern of birth defects from inadvertent first-trimester exposure, but stopping is still the standard approach for most patients.

Call prescriber Before trying to conceive, on missed period, or on a positive home pregnancy test. Also before breastfeeding, as the medicine is not recommended during lactation.

Alcohol

Tell patient Light to moderate alcohol use is generally compatible. Heavy or daily drinking raises the chance of liver irritation and is best avoided while on this medicine.

Call prescriber Yellowing of the skin or eyes, persistent abdominal pain, very dark urine, or unusual fatigue — any of these warrant prompt evaluation regardless of alcohol intake.

Diabetes Risk

Tell patient Statins very slightly raise the chance of being diagnosed with diabetes, mainly in people who were already on the borderline. The protection from heart attacks and strokes is far larger than this small risk, so the medicine is still recommended.

Call prescriber Increased thirst, frequent urination, unexplained weight loss, or persistently elevated home blood-sugar readings (if monitoring is being done).

Ref

Sources

Regulatory (PI / Drug Safety Communications)

ZOCOR (simvastatin) US Prescribing Information. Organon LLC; revised 2023. Accessed via FDA Drugs@FDA. accessdata.fda.gov/drugsatfda_docs/label/2023/019766Orig1s103lbl.pdf Authoritative source for FDA-approved indications, dosing limits, contraindications, drug interactions, and adverse-reaction frequencies cited in this monograph.
FLOLIPID (simvastatin) Oral Suspension US Prescribing Information. Salerno Pharmaceuticals. Available via DailyMed. dailymed.nlm.nih.gov Reference for the oral suspension formulation; note that this label retains “active liver disease” as a contraindication, which differs from the current Zocor tablet PI.
FDA Drug Safety Communication: New restrictions, contraindications, and dose limitations for Zocor (simvastatin) to reduce the risk of muscle injury. June 8, 2011. fda.gov Underlies the 80 mg restriction and the dose caps with amiodarone, calcium channel blockers, and other interacting drugs.
FDA Drug Safety Communication: FDA requests removal of strongest warning against using cholesterol-lowering statins during pregnancy. July 20, 2021. fda.gov The 2021 labeling change removing the pregnancy contraindication for the entire statin class.

Key Clinical Trials

Scandinavian Simvastatin Survival Study Group. Randomised trial of cholesterol lowering in 4444 patients with coronary heart disease: the Scandinavian Simvastatin Survival Study (4S). Lancet. 1994;344(8934):1383-1389. doi:10.1016/s0140-6736(94)90566-5 First statin outcome trial showing a mortality benefit; underpins the secondary-prevention indication.
Heart Protection Study Collaborative Group. MRC/BHF Heart Protection Study of cholesterol lowering with simvastatin in 20,536 high-risk individuals: a randomised placebo-controlled trial. Lancet. 2002;360(9326):7-22. doi:10.1016/S0140-6736(02)09327-3 Demonstrated CV benefit across diabetes, peripheral vascular disease, and prior stroke regardless of baseline LDL-C; basis for broad high-risk indication.
SEARCH Collaborative Group. Intensive lowering of LDL cholesterol with 80 mg versus 20 mg simvastatin daily in 12,064 survivors of myocardial infarction: a double-blind randomised trial. Lancet. 2010;376(9753):1658-1669. doi:10.1016/S0140-6736(10)60310-8 Source for the myopathy and rhabdomyolysis rates that triggered the FDA 2011 restriction on the 80 mg dose.
HPS2-THRIVE Collaborative Group. Effects of extended-release niacin with laropiprant in high-risk patients (HPS2-THRIVE). N Engl J Med. 2014;371(3):203-212. doi:10.1056/NEJMoa1300955 Identified excess myopathy in Chinese patients on simvastatin plus niacin and the absence of CV benefit from niacin add-on therapy.

Guidelines

Grundy SM, Stone NJ, Bailey AL, et al. 2018 AHA/ACC/AACVPR/AAPA/ABC/ACPM/ADA/AGS/APhA/ASPC/NLA/PCNA Guideline on the Management of Blood Cholesterol. Circulation. 2019;139(25):e1082-e1143. doi:10.1161/CIR.0000000000000625 Primary US guideline; classifies simvastatin 20–40 mg as moderate intensity and 10 mg as low intensity.
Mach F, Baigent C, Catapano AL, et al. 2019 ESC/EAS Guidelines for the management of dyslipidaemias. Eur Heart J. 2020;41(1):111-188. doi:10.1093/eurheartj/ehz455 European framework with lower LDL-C targets in very-high-risk patients; supports preferential use of high-intensity statins over simvastatin in these populations.
Newman CB, Preiss D, Tobert JA, et al. Statin Safety and Associated Adverse Events: A Scientific Statement From the American Heart Association. Arterioscler Thromb Vasc Biol. 2019;39(2):e38-e81. doi:10.1161/ATV.0000000000000073 Comprehensive class-wide safety review used here for myopathy framing, observational vs RCT muscle-symptom rates, and diabetes risk discussion.

Mechanistic / Pharmacology / Pharmacogenetics

Cholesterol Treatment Trialists’ (CTT) Collaboration. Efficacy and safety of more intensive lowering of LDL cholesterol: a meta-analysis of data from 170,000 participants in 26 randomised trials. Lancet. 2010;376(9753):1670-1681. doi:10.1016/S0140-6736(10)61350-5 Class-wide meta-analysis underpinning the “lower is better” LDL-C principle and magnitude-of-benefit framing in this monograph.
Karlson BW, Palmer MK, Nicholls SJ, Lundman P, Barter PJ. Variability of low-density lipoprotein cholesterol response with different doses of atorvastatin, rosuvastatin, and simvastatin: results from VOYAGER. Eur Heart J Cardiovasc Pharmacother. 2016;2(4):212-217. doi:10.1093/ehjcvp/pvw006 Source for the simvastatin LDL-C reduction data (28% at 10 mg to 46% at 80 mg) used throughout the monograph.
SEARCH Collaborative Group. SLCO1B1 variants and statin-induced myopathy — a genomewide study. N Engl J Med. 2008;359(8):789-799. doi:10.1056/NEJMoa0801936 Established the SLCO1B1 (OATP1B1) variant rs4149056 as the major genetic determinant of simvastatin-induced myopathy risk.