Drug-drug interactions
Drug-drug pairs with clinical significance. Each pair includes mechanism, management, and links to international clinical guidelines (ESC, AHA/ACC, FDA, AGS Beers, Stockley's, Lexicomp)
Checker: pick two drugs →110 of 110 shown
- Major
Enalapril × Espironolactona
Dual blockade of the renin-angiotensin-aldosterone system.
- Major
co-trimoxazole × Enalapril
- Minor
Atorvastatina × Clopidogrel
An early study by Lau et al.
- Major
Amiodarona × Warfarina
Amiodarone potently inhibits CYP2C9 (the main enzyme metabolizing S-warfarin) and, to a lesser extent, CYP3A4 (R-warfarin metabolism).
- Major
Atorvastatina × Warfarina
Atorvastatin weakly inhibits CYP3A4 and CYP2C9.
- Major
Amiodarona × Apixabán
Amiodarone inhibits CYP3A4 and P-glycoprotein – apixaban exposure rises by approximately 40–50 %.
- Critical
Apixabán × Ketoconazole
- Major
Paracetamol × Warfarina
Paracetamol above 2 g/day for more than 7 days raises INR by 1–3 units.
- Major
Amlodipino × Simvastatina
Amlodipine moderately inhibits CYP3A4 – simvastatin exposure rises 30–80 %, and the risk of myopathy and rhabdomyolysis increases.
- Major
Clopidogrel × Warfarina
Additive antithrombotic effect: warfarin in the coagulation cascade plus clopidogrel at the platelet P2Y12 receptor.
- Major
diazepam × Tramadol
- Major
Amiodarona × Atorvastatina
Amiodarone inhibits CYP3A4, which partially metabolizes atorvastatin.
- Major
Ácido acetilsalicílico × Apixabán
Additive antithrombotic action: apixaban + aspirin increases major bleeding risk roughly 1.
- Major
Apixabán × Clopidogrel
Additive antithrombotic effect on two levels: apixaban blocks factor Xa while clopidogrel inhibits platelet aggregation.
- Major
Ácido acetilsalicílico × Furosemida
Dual mechanism.
- Major
Ácido acetilsalicílico × Espironolactona
Aspirin's NSAID effect reduces prostaglandin-dependent renal perfusion and blunts the diuretic and natriuretic action of spironolactone.
- Minor
Metronidazol × Paracetamol
No direct pharmacokinetic interaction.
- Major
Ácido acetilsalicílico × Warfarina
Additive antithrombotic effect at two levels: warfarin inhibits clotting factors while aspirin blocks platelet aggregation and simultaneously damages gastric mucosa (antiprostaglandin effect).
- Major
digoxin × Metoprolol
Additive AV conduction slowing and heart rate reduction.
- Major
digoxin × Hidroclorotiazida
Thiazides cause hypokalemia and hypomagnesemia.
- Major
dabigatran × dronedarone
- Critical
linezolid × Sertralina
- Major
Bisoprolol × verapamil
- Major
Amiodarona × Sertralina
Both drugs prolong the QT interval (amiodarone strongly via IKr potassium channel blockade; sertraline modestly).
- Major
Hidroclorotiazida × Losartán
Synergistic BP reduction, a target combination in hypertension (losartan/hydrochlorothiazide fixed-dose product).
- Critical
linezolid × Tramadol
- Major
carbamazepine × Warfarina
- Major
carbamazepine × Ethinylestradiol
- Major
digoxin × verapamil
- Major
Amiodarona × clarithromycin
- Moderate
Amlodipino × Atorvastatina
Amlodipine weakly inhibits CYP3A4 – atorvastatin concentration rises by about 18 %.
- Moderate
Amlodipino × Enalapril
Synergistic BP reduction via two mechanisms: amlodipine causes vasodilation, enalapril blocks the RAAS.
- Moderate
Amlodipino × Losartán
Synergistic BP reduction, a target hypertension combination.
- Moderate
Enalapril × Metformina
ACE inhibitors improve tissue insulin sensitivity and potentiate metformin's glucose-lowering effect.
- Critical
clarithromycin × colchicine
- Major
Levotiroxina sódica × Warfarina
Thyroid hormones accelerate catabolism of vitamin K-dependent clotting factors.
- Moderate
Enalapril × Metoprolol
A target combination in HFrEF and hypertension – synergistic BP and pre/afterload reduction.
- Moderate
Furosemida × Espironolactona
Opposing effects on potassium: furosemide depletes potassium, spironolactone retains it.
- Moderate
Losartán × Metoprolol
A target combination in HF and hypertension.
- Moderate
Furosemida × Hidroclorotiazida
Sequential nephron blockade: furosemide acts in the loop of Henle, the thiazide in the distal tubule.
- Moderate
Amiodarona × Furosemida
Furosemide causes hypokalemia and hypomagnesemia – increasing myocardial sensitivity to amiodarone's QT-prolonging effect.
- Moderate
Furosemida × Sertralina
Both drugs can cause hyponatremia (furosemide via natriuresis, sertraline via an SIADH-like mechanism).
- Minor
Metformina × Omeprazol
Omeprazole inhibits intestinal OCT1 – metformin absorption rises slightly.
- Minor
Amoxicilina × Levotiroxina sódica
Amoxicillin can interfere with intestinal absorption of levothyroxine when taken simultaneously – clinically insignificant when administration is separated.
- Minor
Atorvastatina × Levotiroxina sódica
Hypothyroidism by itself raises LDL.
- Moderate
Atorvastatina × Omeprazol
Omeprazole weakly inhibits CYP3A4 – atorvastatin exposure rises modestly (10–20 %).
- Major
Amiodarona × Metoprolol
Dual mechanism: 1) additive AV conduction slowing and heart rate reduction (amiodarone non-competitively blocks β-receptors, metoprolol selectively blocks β1); 2) amiodarone inhibits CYP2D6, doubling metoprolol concentration.
- Major
Enalapril × Furosemida
In patients with activated RAAS (significant hypovolemia from aggressive diuresis, severe HF), the first ACE-inhibitor dose can cause an abrupt BP drop with syncope and acute kidney injury.
- Moderate
Ácido acetilsalicílico × Ciprofloxacino
Older experimental data suggested that NSAIDs combined with fluoroquinolones increase CNS excitability and seizure risk (via fluoroquinolone-mediated GABA-A receptor antagonism with possible NSAID potentiation).
- Major
Ciprofloxacino × Sertralina
Additive QT prolongation: sertraline modestly and ciprofloxacin modestly.
- Major
Fluconazol × Warfarina
- Moderate
Ciprofloxacino × Omeprazol
Ciprofloxacin is better absorbed in an acidic gastric environment.
- Minor
Amoxicilina × Metronidazol
A target combination in triple/quadruple Helicobacter pylori eradication regimens (Maastricht VI / Florence Consensus 2022, Kyoto Global Consensus, Russian Ministry of Health 2024 guidelines).
- Major
Fluoxetina × Tramadol
- Critical
Losartán × Espironolactona
Same as the ACE-inhibitor/spironolactone pair: the ARB blocks AT1 receptors and lowers aldosterone synthesis, while spironolactone blocks the mineralocorticoid receptor.
- Critical
Amiodarona × digoxin
Amiodarone inhibits intestinal and renal P-glycoprotein – plasma digoxin concentration rises 1.
- Major
Sertralina × Tramadol
- Major
Ibuprofeno × Metotrexato
- Critical
Enalapril × Losartán
Dual RAAS blockade at two levels: enalapril blocks angiotensin II formation, losartan blocks the binding of residual angiotensin II to the AT1 receptor.
- Major
Simvastatina × Warfarina
Simvastatin inhibits CYP3A4 and to a lesser extent CYP2C9, raising warfarin concentration.
- Major
Sertralina × Warfarina
Dual mechanism: 1) sertraline inhibits serotonin reuptake in platelets, depleting platelet serotonin and reducing aggregation; 2) moderate CYP2C9 inhibition raises warfarin concentration and INR.
- Major
Apixabán × Sertralina
SSRIs deplete platelet serotonin and impair primary hemostasis.
- Major
Ácido acetilsalicílico × Clopidogrel
Additive antiplatelet action: aspirin inhibits COX-1 → thromboxane, clopidogrel blocks the P2Y12 receptor.
- Major
Amoxicilina × Warfarina
Broad-spectrum antibiotics eliminate gut flora that synthesize vitamin K2 – reducing vitamin K availability for hepatic γ-carboxylation.
- Major
Ácido acetilsalicílico × Losartán
Same as the aspirin/ACE-inhibitor pair: aspirin's NSAID effect blunts renal vasodilation, and patients with CKD or hypovolemia may develop acute kidney injury.
- Major
Furosemida × Losartán
Same as the ACE-inhibitor/furosemide pair: in a hypovolemic patient the first sartan dose can cause an abrupt BP drop and acute kidney injury.
- Major
Ácido acetilsalicílico × Enalapril
Aspirin's COX inhibition reduces renal prostaglandin-mediated vasodilation.
- Major
Enalapril × Hidroclorotiazida
Synergistic BP reduction (a target combination in hypertension – even an enalapril/hydrochlorothiazide fixed-dose product exists).
- Major
Hidroclorotiazida × Metformina
Thiazides cause dose-dependent hyperglycemia and insulin resistance (especially at doses ≥ 25 mg/day) via hypokalemia and reduced insulin secretion.
- Moderate
Losartán × Metformina
Sartans, like ACE inhibitors, improve tissue insulin sensitivity.
- Moderate
Amlodipino × Metoprolol
A target combination in angina and hypertension.
- Moderate
digoxin × Espironolactona
Spironolactone moderately inhibits P-glycoprotein – digoxin concentration rises by 20–30 %.
- Moderate
Clopidogrel × Sertralina
Two effects: 1) clopidogrel blocks aggregation at the P2Y12 receptor while sertraline impairs primary hemostasis by inhibiting platelet serotonin reuptake; 2) sertraline weakly inhibits CYP2C19 – clopidogrel activation is slightly reduced.
- Moderate
Hidroclorotiazida × Espironolactona
Opposing effects on potassium: thiazide depletes, spironolactone retains.
- Moderate
Hidroclorotiazida × Sertralina
Thiazides are one of the commonest drug causes of hyponatremia in older adults (via an SIADH-like mechanism plus natriuresis).
- Moderate
Amiodarona × Hidroclorotiazida
Same as the amiodarone/furosemide pair: thiazide-induced hypokalemia and hypomagnesemia raise amiodarone's arrhythmogenic potential.
- Moderate
Omeprazol × Sertralina
Omeprazole inhibits CYP2C19 – sertraline concentration rises by roughly 40 %.
- Major
Amiodarona × Ciprofloxacino
Additive QT prolongation: amiodarone strongly blocks IKr potassium channels and ciprofloxacin does the same more mildly.
- Moderate
Ciprofloxacino × digoxin
In 10–15 % of patients, gut flora (mainly Eubacterium lentum) metabolize part of digoxin into inactive products.
- Critical
Ácido acetilsalicílico × Warfarina
Additive antithrombotic effect plus platelet aggregation inhibition.
- Moderate
Clopidogrel × Omeprazol
Omeprazole is a potent CYP2C19 inhibitor, the key enzyme for clopidogrel bioactivation.
- Major
Metronidazol × Warfarina
Metronidazole stereospecifically inhibits CYP2C9, the enzyme that metabolizes S-warfarin (the more potent enantiomer).
- Major
Amiodarona × digoxin
- Major
Enalapril × Ibuprofeno
- Major
Metronidazol × Warfarina
- Major
Ibuprofeno × Warfarina
- Major
Amiodarona × Azitromicina
- Moderate
Levotiroxina sódica × Omeprazol
Levothyroxine sodium requires gastric acidity to dissolve.
- Moderate
Ácido acetilsalicílico × Ibuprofeno
- Major
Clopidogrel × Ibuprofeno
- Major
Clopidogrel × Warfarina
- Major
Amiodarona × Simvastatina
Amiodarone inhibits CYP3A4, the enzyme responsible for simvastatin metabolism.
- Major
Ibuprofeno × lithium
- Major
Ciprofloxacino × theophylline
- Critical
nitroglycerin × sildenafil
- Major
Hypericum perforatum × Sertralina
- Critical
Ketoconazole × Rivaroxabán
- Critical
clarithromycin × Simvastatina
- Major
Iopromide × Metformina
- Major
digoxin × Furosemida
Furosemide causes potassium and magnesium loss.
- Moderate
Calcium carbonate × Levotiroxina sódica
- Major
clarithromycin × haloperidol
- Major
Ethinylestradiol × rifampicin
- Major
rifampicin × Warfarina
- Major
clarithromycin × Ciclosporin
- Major
Furosemida × gentamicin
- Major
Furosemida × lithium
- Moderate
Glibenclamide × propranolol
- Moderate
Ciprofloxacino × Metformina
Fluoroquinolones disrupt glucose homeostasis – they can cause both hypoglycemia (especially in older patients on glucose-lowering therapy) and hyperglycemia.
- Major
Ciprofloxacino × Warfarina
Dual mechanism: 1) ciprofloxacin is a moderate CYP1A2 inhibitor and weak CYP3A4 inhibitor, raising R-warfarin concentration; 2) elimination of gut flora reduces vitamin K2 synthesis.