Supplements That Interact with Medications: The Complete Evidence-Based Guide

1. St. John's Wort: The Biggest Offender

St. John's Wort (Hypericum perforatum) is sold as a natural remedy for depression and anxiety. It is also the most dangerous supplement in terms of drug interactions, capable of reducing the effectiveness of dozens of critical medications. For full supplement background, see Health Britannica's St. John's Wort profile.

The mechanism: St. John's Wort is a potent inducer of both the CYP3A4 enzyme system and the P-glycoprotein (P-gp) drug transporter. "Inducing" these systems means St. John's Wort causes your body to produce more of these drug-metabolizing enzymes and transporters, which accelerates the breakdown and excretion of other medications. The result: lower blood levels of those medications, often below the therapeutic range.

This is the opposite of the grapefruit interaction (which inhibits CYP3A4 and raises drug levels). St. John's Wort lowers drug levels, which can be equally dangerous when the medication being reduced is critical for your health. For the grapefruit side of the CYP3A4 equation, see our grapefruit drug interactions guide.

Medications affected:

• Oral contraceptives: St. John's Wort can reduce the effectiveness of hormonal birth control, leading to unintended pregnancies. Multiple case reports document this outcome. The mechanism: CYP3A4 induction accelerates the metabolism of ethinyl estradiol and progestins. Source: FDA MedWatch safety communication.
• Warfarin and other anticoagulants: Reduced warfarin levels can lead to subtherapeutic INR, increasing the risk of blood clots, stroke, and pulmonary embolism. A study in The Lancet (2000) documented significant INR reductions in patients who started St. John's Wort while on warfarin.
• Immunosuppressants (cyclosporine, tacrolimus): Organ transplant recipients who take St. John's Wort can experience dramatic drops in immunosuppressant blood levels, leading to acute organ rejection. Case reports in the Annals of Internal Medicine and Transplantation have documented kidney and heart transplant rejections attributed to St. John's Wort use.
• HIV antiretrovirals (indinavir, nevirapine, efavirenz): CYP3A4 induction reduces protease inhibitor levels, potentially causing treatment failure and viral resistance. The NIH Office of Dietary Supplements explicitly warns against this combination, and peer-reviewed pharmacokinetic data on PubMed document significant indinavir AUC reductions.
• SSRIs and SNRIs: Paradoxically, St. John's Wort can also cause serotonin syndrome when combined with prescription antidepressants, because it has serotonergic activity of its own while simultaneously altering their metabolism.
• Statins, calcium channel blockers, benzodiazepines, cancer drugs: All CYP3A4 substrates are potentially affected.

Bottom line: If you take any prescription medication, do not take St. John's Wort without explicit approval from your prescriber. The interaction profile is too broad and too dangerous. If you are seeking natural approaches for mood support, discuss alternatives with your healthcare provider. Health Britannica covers evidence-based alternatives for mood support that do not carry the same interaction risks.

2. Fish Oil (Omega-3 Fatty Acids) + Blood Thinners

Fish oil supplements containing EPA and DHA are among the most popular supplements in the United States, taken by millions for cardiovascular health, triglyceride reduction, and anti-inflammatory effects. For detailed supplement information, see Health Britannica's fish oil guide.

The interaction: Omega-3 fatty acids have antiplatelet and antithrombotic effects. They reduce platelet aggregation (the clumping of blood cells that forms clots) through mechanisms involving thromboxane A2 and prostacyclin pathways. When combined with anticoagulants (warfarin, apixaban, rivaroxaban) or antiplatelet drugs (aspirin, clopidogrel), fish oil can increase bleeding risk.

How significant is it? The clinical significance depends heavily on dose. Standard supplemental doses (1-2 grams of omega-3s daily) appear to carry minimal additional bleeding risk based on meta-analyses published in Circulation (2019). However, prescription-strength doses (4 grams daily, such as Lovaza or Vascepa) produce more significant antiplatelet effects and warrant closer monitoring when combined with anticoagulants.

What to do:

• If you take warfarin: Inform your anticoagulation clinic about fish oil use. Your INR may need more frequent monitoring.
• If you take DOACs (apixaban, rivaroxaban): Mention fish oil to your prescriber. The added bleeding risk is generally small at standard supplement doses but worth noting.
• Watch for signs of increased bleeding: unusual bruising, prolonged bleeding from cuts, blood in urine or stool, nosebleeds.
• If you take high-dose prescription omega-3s (4 g/day): This is essentially a drug, not a supplement, and your prescriber should be managing it alongside your other medications.

3. Calcium + Thyroid Medications (Levothyroxine)

Levothyroxine (Synthroid, Levoxyl) is one of the most prescribed medications in the United States, with over 100 million prescriptions annually. Calcium supplements are taken by tens of millions of Americans, primarily women, for bone health. The overlap is enormous. For calcium supplement details, see Health Britannica's calcium guide.

The interaction: Calcium binds to levothyroxine in the gastrointestinal tract, forming an insoluble complex that prevents the thyroid medication from being absorbed. Studies in Thyroid (2001) and the Journal of Clinical Endocrinology and Metabolism (2006) demonstrated that concurrent calcium administration reduced levothyroxine absorption by 20-25%. For a patient whose thyroid dose has been carefully titrated, a 20-25% reduction can shift them from euthyroid (normal) to hypothyroid (undertreated).

The solution is simple: Separate them by at least 4 hours. Take levothyroxine first thing in the morning on an empty stomach (the standard recommendation). Take calcium supplements at lunch, dinner, or bedtime. This timing separation allows the levothyroxine to be fully absorbed before calcium enters the GI tract.

Other minerals that bind levothyroxine: Iron, magnesium, and aluminum (from antacids) produce the same binding interaction. If you take a multivitamin containing these minerals, take it 4 hours after your levothyroxine.

Full interaction details: Levothyroxine and calcium

4. Magnesium + Antibiotics

Magnesium supplements are widely used for muscle cramps, sleep, migraine prevention, and general wellness. For detailed magnesium information, see Health Britannica's magnesium guide.

The interaction: Magnesium (like calcium and iron) is a divalent cation that chelates (binds to) certain antibiotic molecules in the GI tract, forming insoluble complexes that pass through the body without being absorbed. Two major antibiotic classes are affected:

• Fluoroquinolones (ciprofloxacin, levofloxacin, moxifloxacin): Magnesium can reduce fluoroquinolone absorption by 30-50%. This is not a trivial reduction. Subtherapeutic antibiotic levels can lead to treatment failure and, critically, the development of antibiotic-resistant bacteria. The FDA-approved labels for all fluoroquinolones include a specific warning to avoid concurrent use with magnesium-containing products.
• Tetracyclines (doxycycline, minocycline, tetracycline): Similar chelation effect. Absorption can be reduced by 50-80%. Take tetracyclines at least 2 hours before or 6 hours after any magnesium supplement.

Magnesium and blood pressure medications: Magnesium supplements can lower blood pressure independently. When combined with prescription antihypertensive medications (ACE inhibitors, ARBs, calcium channel blockers), the blood pressure-lowering effects can be additive, potentially causing dizziness, lightheadedness, or falls, especially in elderly patients. This is generally manageable but worth mentioning to your prescriber.

Related: Ciprofloxacin and antacids interaction

5. Vitamin K + Warfarin

The vitamin K-warfarin interaction is one of the most important in all of clinical medicine. For vitamin K background, see Health Britannica's vitamin K guide.

The mechanism: Warfarin works by inhibiting vitamin K epoxide reductase, the enzyme that recycles vitamin K into its active form. Active vitamin K is essential for producing clotting factors II, VII, IX, and X in the liver. By blocking vitamin K recycling, warfarin reduces clotting factor production and prevents dangerous blood clots.

Vitamin K supplements directly counteract warfarin's mechanism. Flooding the body with vitamin K provides the raw material for clotting factor production through an alternative pathway, effectively overwhelming warfarin's inhibition. The result: a rapid increase in clotting ability, which can cause the patient's INR to drop below the therapeutic range, putting them at risk for stroke, deep vein thrombosis, or pulmonary embolism.

The nuance: The issue is not just vitamin K supplements. Dietary vitamin K from food (leafy green vegetables like kale, spinach, broccoli, Brussels sprouts) also affects warfarin. The clinical guidance is not to avoid vitamin K entirely, but to keep your vitamin K intake consistent from day to day. Sudden increases or decreases in vitamin K consumption cause INR fluctuations that are difficult to manage.

What to do:

• Do not take vitamin K supplements while on warfarin unless specifically directed by your doctor.
• Do not avoid green vegetables. Instead, eat a consistent amount each week.
• Be cautious with multivitamins that contain vitamin K. Many do, and the amounts vary between brands.
• If you change your diet significantly (starting a keto diet, going vegan, beginning a green smoothie habit), alert your anticoagulation clinic so they can check your INR.

Full interaction details: Warfarin and vitamin K

6. Iron + Levothyroxine (and Other Medications)

Iron supplements are commonly prescribed for iron-deficiency anemia, particularly in women of reproductive age, pregnant women, and patients with chronic kidney disease. For iron supplement details, see Health Britannica's iron supplement guide.

The interaction: Like calcium and magnesium, iron is a mineral that chelates medications in the GI tract. The medications most affected by iron include:

• Levothyroxine: Iron reduces levothyroxine absorption by 50-75% when taken simultaneously. This is an even larger effect than calcium. A study in the Journal of Clinical Endocrinology and Metabolism found that patients who started iron supplements while on levothyroxine had significant increases in TSH (indicating hypothyroidism) within 6-8 weeks. Separate these by at least 4 hours.
• Fluoroquinolone antibiotics: Iron reduces ciprofloxacin absorption by 50-65%. Same chelation mechanism as magnesium.
• Tetracycline antibiotics: Iron can reduce tetracycline absorption by up to 90%. This is one of the most dramatic absorption interactions in pharmacology.
• Levodopa (for Parkinson's disease): Iron chelates levodopa, reducing its absorption and effectiveness. This is particularly concerning because levodopa dose adjustments can take weeks to stabilize.
• Bisphosphonates (alendronate, risedronate): Iron reduces absorption. Take bisphosphonates at least 2 hours before iron.
• ACE inhibitors (captopril): Iron can reduce captopril absorption and may affect its blood pressure-lowering efficacy.

The timing rule for iron: Take iron supplements at least 2 hours away from any chelation-sensitive medication. For levothyroxine, the recommendation is 4 hours. Many clinicians suggest taking iron in the evening if you take morning medications, or vice versa.

7. CoQ10 + Blood Pressure and Blood-Thinning Medications

Coenzyme Q10 (ubiquinone) is a popular supplement taken for heart health, statin-associated muscle pain, and general energy support. For CoQ10 background, see Health Britannica's CoQ10 guide.

The interactions:

CoQ10 + blood pressure medications: CoQ10 has modest blood pressure-lowering effects (approximately 11 mmHg systolic and 7 mmHg diastolic, according to a meta-analysis in the Journal of Human Hypertension, 2007). When added to prescription antihypertensive therapy, this additional reduction can cause symptomatic hypotension (dizziness, lightheadedness, fatigue), particularly in patients whose blood pressure is already well-controlled. The interaction is generally manageable with blood pressure monitoring and possible dose adjustment of the prescription medication.

CoQ10 + warfarin: CoQ10 is structurally similar to vitamin K2. Theoretically, it could interfere with warfarin's anticoagulant effect, though the clinical evidence is mixed. Some case reports describe decreased INR in patients who started CoQ10 while on warfarin. The mechanism may involve CoQ10 providing a low-level vitamin K-like effect or affecting warfarin metabolism. If you take warfarin and want to start CoQ10, inform your anticoagulation clinic and monitor your INR closely during the first few weeks.

CoQ10 + statins: This interaction is actually why many people take CoQ10 in the first place. Statins inhibit HMG-CoA reductase, which sits upstream of CoQ10 in the mevalonate pathway. Statin therapy reduces endogenous CoQ10 production. Some patients supplement with CoQ10 to address statin-associated myalgia (muscle pain). This is not a harmful interaction. It is a complementary use, though the evidence for CoQ10 relieving statin myalgia is mixed (a 2018 Cochrane review found insufficient evidence to confirm or deny the benefit).