Do I need a prescription for Dronedarone 400mg tablets?

Dronedarone 400mg tablets is classified as a Valid as a prescribable product in the UK. However, always consult a pharmacist or doctor before use. (Source: NHS dm+d)

What are the brand names for Dronedarone 400mg tablets?

Dronedarone 400mg tablets is the generic name. It is available under brand names including: Dronedarone 400mg tablets, Dronedarone 400mg tablets, Dronedarone 400mg tablets, Dronedarone 400mg tablets, Dronedarone 400mg tablets and 7 more. (Source: NHS dm+d — Actual Medicinal Products)

Dronedarone 400mg tablets

Prescription only

Requires a prescription from a doctor or prescriber

Tablet

400mg

Oral

Dronedarone is a Class III antiarrhythmic drug that works to restore the normal sinus rhythm in patients with paroxysmal or persistent atrial fibrillation.

Active ingredients:

Dronedarone

BNF classificationBrowse formulary

Where this medicine sits in the British National Formulary — the UK's standard prescribing reference

BNF 02.03.02

ATC classificationBrowse ATC index

International classification by the WHO, grouping medicines by the organ system they act on

ATC C01BD07

Chemical classBrowse classes

Classification based on the molecule's chemical structure and properties

Check interactions for Dronedarone

No active safety alerts

Official documents, adverse reaction reporting, and safety monitoring

Report a side effect

Submit a Yellow Card report to the MHRA

Official medicine documents

Yellow Card

Report side effects (MHRA)

Drug safety updates

MHRA alerts for Dronedarone

Source: MHRA Products DatabaseOGL 3.0

Updated 3 months ago(16 Jan 2026)

Safety monitoring data

Yellow Card reports

MHRA

The MHRA Yellow Card scheme collects reports of suspected side effects from healthcare professionals and patients. View the Drug Analysis Profile (iDAP) for real-world adverse reaction data.

View Drug Analysis Profile

Suspected adverse reactions reported for Dronedarone

Browse all iDAP reports

Interactive Drug Analysis Profiles for all medicines

Report a side effect

Submit a Yellow Card report to the MHRA

Data from the MHRA Yellow Card scheme. A reported reaction does not necessarily mean the medicine caused it. Contains public sector information licensed under the Open Government Licence v3.0.

EudraVigilance

EMA

The European Medicines Agency (EMA) collects suspected adverse reaction reports from across the EU/EEA through the EudraVigilance system. Search for safety data on this medicine.

View EudraVigilance report

Suspected adverse reactions reported for Dronedarone

About EudraVigilance

Learn about EU pharmacovigilance and safety monitoring

EudraVigilance data is published by the European Medicines Agency (EMA). A suspected adverse reaction is not necessarily caused by the medicine.

12 branded products available

12 productsShow details

12 products

Possibly available on the UK marketDiscontinuedAvailability per NHS dm+d

MHRA licensed products

View all licensed products for Dronedarone on the MHRA register

Multaq 400mg tablets

Sanofi

Multaq 400mg tablets

Sigma Pharmaceuticals Plc

Multaq 400mg tablets

Pharmaram Ltd

Dronedarone 400mg tablets

Aristo Pharma Ltd

Dronedarone 400mg tablets

Alliance Healthcare (Distribution) Ltd

Dronedarone 400mg tablets

Accord-UK Ltd

Dronedarone 400mg tablets

A A H Pharmaceuticals Ltd

Dronedarone 400mg tablets

Milpharm Ltd

Dronedarone 400mg tablets

Necessity Supplies Ltd

Multaq 400mg tablets

Waymade Healthcare Plc

Discontinued

Dronedarone 400mg tablets

Colorama Pharmaceuticals Ltd

Discontinued

Dronedarone 400mg tablets

DE Pharmaceuticals

Discontinued

Source: NHS dm+dOGL 3.0

Updated about 1 month ago(1 Mar 2026)

Price & daily doseShow details

£17.30indicative price

This is the NHS Drug Tariff indicative price used for reimbursement purposes. It may not reflect the price paid by patients or pharmacies.

View full Drug Tariff

Source: NHS Drug Tariff via NHSBSA. Derived from dm+d VMPP (Virtual Medicinal Product Pack) pricing data. Contains public sector information licensed under the Open Government Licence v3.0.

WHO defined daily dose (DDD)

800 mg

Not a recommended dose. The DDD is the assumed average maintenance dose per day for a drug used for its main indication in adults. It is a statistical measure used for research and comparison purposes only.

Source: WHO Collaborating Centre for Drug Statistics Methodology, distributed via NHS dm+d BNF mapping files. Contains public sector information licensed under the Open Government Licence v3.0.

Therapeutically similar medicines

10 similarShow details

Dofetilide 125microgram capsules

Capsule

Same therapeutic group

Dofetilide 250microgram capsules

Capsule

Same therapeutic group

Dofetilide 500microgram capsules

Capsule

Same therapeutic group

Amiodarone 10mg/5ml oral suspension

Oral suspension

10mg/5ml

Same therapeutic group

Amiodarone 10mg/5ml oral solution

Oral solution

10mg/5ml

Same therapeutic group

Similarity based on WHO Anatomical Therapeutic Chemical (ATC) classification and NHS BNF section grouping. Source data: NHS dm+d via TRUD (OGL v3.0), WHO ATC/DDD Index.

NHS prescribing volume and spending trends

Show details

Loading prescribing data...

Clinical guidelines and formulary information

British National Formulary

Dronedarone

BNF

Drug monograph — bnf.nice.org.uk

Source: British National Formulary, NICE. Joint Formulary Committee. Contains public sector information licensed under the Open Government Licence v3.0.

NICE clinical guidance(3)

Dronedarone for the treatment of non-permanent atrial fibrillation (TA197)

TA197

Technology appraisal

Updated Dec 2012

Atrial fibrillation: diagnosis and management (NG196)

NG196

NICE guideline

Updated Jun 2021

Edoxaban for preventing stroke and systemic embolism in people with non-valvular atrial fibrillation (TA355)

TA355

Technology appraisal

Updated Jul 2021

Source: National Institute for Health and Care Excellence (NICE). Contains public sector information licensed under the Open Government Licence v3.0.

Check stock at pharmacies and supply information

Show details

Pharmacy stock checkers

Search for this medicine at major UK pharmacy chains. These links open the retailer's own website — results depend on their current online catalogue.

Boots

Search products

Click & collectNHS

Lloyds

Search products

DeliveryNHS

P2U

Pharmacy2U

Search products

DeliveryNHS

Supply & product information

Official product databases and supply status monitoring

Shortages info

NHS Specialist Pharmacy Service (SPS)

emc product search

Discontinuations & alternatives for Dronedarone

Pharmacy links redirect to the retailer's own search and do not represent real-time stock levels. emc (electronic medicines compendium) is operated by Datapharm Ltd. Shortage information sourced from NHS Specialist Pharmacy Service (SPS), sps.nhs.uk.

Codes for healthcare professionals and prescribing systems

Show details

These codes are used by healthcare IT systems and prescribers to identify this medicine.

NHS UK identifiers

SNOMED CT

39691711000001107

dm+d ID

39691711000001107

VTM (Virtual Therapeutic Moiety)

775703009

VMP (Virtual Medicinal Product)

39691711000001107

BNF code

02030200

International identifiers

ATC code — Anatomical Therapeutic Chemical (WHO)

C01BD07

Browse tools

dm+d Browser

NHSBSA medicines dictionary lookup

SNOMED CT and dm+d codes from NHS TRUD (Technology Reference data Update Distribution), licensed under the Open Government Licence v3.0. BNF codes from NHS Business Services Authority (NHSBSA). ATC codes from the WHO Collaborating Centre for Drug Statistics Methodology (whocc.no).

Active and completed clinical studies from ClinicalTrials.gov

Show details

Searching UK clinical trials...

Source: ClinicalTrials.gov, a database of the U.S. National Library of Medicine (NLM), National Institutes of Health (NIH). Data accessed via ClinicalTrials.gov API v2. Trial information is provided for research purposes and does not constitute medical advice.

Pharmacology and chemical data from DrugBank

go.drugbank.com

Key facts

Drug status

Approved

Major interactions

4 found

Half-life

13 to 19 hours

Mechanism

Atrial fibrillation is the most common type of arrhythmia that is caused by abnormal electrical activity in the atria.

Food interactions

3 warnings

Human targets

25 targets

Data: DrugBank · CC BY-NC 4.0

Pharmacokinetics at a glance

Absorption

70%

Dronedarone is well absorbed after oral administration (>70%).
[A34604]…

Half-life

13 to 19 hours

The elimination half life ranges from 13 to 19 hours.
[L8699]

Protein binding

99.7%

The in vitro plasma protein binding of dronedarone and its N-debutyl metabolite is 99.7%…

Volume of distribution

1200 to 1400 L

The volume of distribution at steady-state ranges from 1200 to 1400 L following intravenous administration.
[L8699]

Metabolism

Dronedarone predominantly undergoes CYP3A-mediated hepatic metabolism.…

Elimination

84%

Following oral administration, about 84% of the labeled dose is excreted in feces and 6% is excreted in urine, mainly as metabolites.…

Clearance

130 to 150 L/h

Following intravenous administration, the clearance ranged from 130 to 150 L/h.
[L8699]

Pharmacokinetic data: DrugBank · CC BY-NC 4.0

Status:

Approved

Investigational

Small molecule

About this compound

Dronedarone is a Class III antiarrhythmic drug that works to restore the normal sinus rhythm in patients with paroxysmal or persistent atrial fibrillation. Atrial fibrillation is a common sustained arrhythmia where the treatment primarily focuses on stroke prevention and symptom management. It is managed by rate control, rhythm control, prevention of thromboembolic events, and treatment of the underlying disease.[A34604] Similar to [amiodarone], dronedarone is a multichannel blocker that works to control rhythm and rate in atrial fibrillation.[A186071] It meets criteria of all four Vaughan Williams antiarrhythmic drug classes by blocking sodium, potassium, and calcium ion channels and inhibiting β-adrenergic receptors.[A34604][L8699]

Dronedarone is a related benzofuran compound to amiodarone but its chemical structure lacks iodine moieties which are associated with amiodarone-induced thyroid problems.[A34604,T28] Additionally, the methyl sulfonyl group in its structure renders dronedarone to be more lipophilic with a shorter half-life than amiodarone.[A34604] This ultimately leads to reduced tissue accumulation of the drug and decreased risk for organ toxicities, such as thyroid and pulmonary toxicities.T28 Commonly marketed as Multaq®, dronedarone was approved by the FDA in July 2009 and Health Canada in August 2009. A safety concern for the risk of drug-induced hepatocellular injury has been issued following marketing of dronedarone.[L8800]

Properties:

solid

Avg. mass: 556.76 Da

DrugBank indication

Dronedarone is indicated for the management of atrial fibrillation (AF) in patients in sinus rhythm with a history of paroxysmal or persistent AF to reduce the risk of hospitalization.
[L8699]

Also known as(217)

Dronedarona

Dronedarone

N-(2-butyl-3-(4-(3-(dibutylamino)propoxy)benzoyl)-5-benzofuranyl)-methanesulfonamide

N-(2-butyl-3-(p-(3-(dibutylamino)propoxy)benzoyl)-5-benzofuranyl)methanesulfonamide

ADRA1C

Alpha-1A adrenoceptor

Alpha-1A adrenoreceptor

Alpha-1C adrenergic receptor

Dosage forms(5)

Tablet (Oral) — 400 mg

Tablet, film coated (Oral) — 400 mg/1

Tablet, coated (Oral) — 400 mg

Tablet, film coated (Oral) — 400 mg

Tablet (Oral) — 426.000 mg

Molecular properties(19)

Drug interactions(1714)

Known interactions with other medications. Always consult a healthcare professional.

Afatinib

Unknown severity

DB08916

The serum concentration of Afatinib can be increased when it is combined with Dronedarone.

Check this interaction

Modafinil

Moderate

DB00745

The metabolism of Dronedarone can be increased when combined with Modafinil.

Check this interaction

Armodafinil

Moderate

DB06413

The metabolism of Dronedarone can be increased when combined with Armodafinil.

Check this interaction

Bosutinib

Unknown severity

DB06616

The serum concentration of Bosutinib can be increased when it is combined with Dronedarone.

Check this interaction

Brentuximab vedotin

Unknown severity

DB08870

The serum concentration of Brentuximab vedotin can be increased when it is combined with Dronedarone.

Check this interaction

Cyclosporine

Unknown severity

DB00091

The serum concentration of Dronedarone can be increased when it is combined with Cyclosporine.

Check this interaction

Edoxaban

Unknown severity

DB09075

The serum concentration of Edoxaban can be increased when it is combined with Dronedarone.

Check this interaction

Ledipasvir

Unknown severity

DB09027

The serum concentration of Ledipasvir can be increased when it is combined with Dronedarone.

Check this interaction

Naloxegol

Unknown severity

DB09049

The serum concentration of Naloxegol can be increased when it is combined with Dronedarone.

Check this interaction

Pazopanib

Unknown severity

DB06589

The serum concentration of Pazopanib can be increased when it is combined with Dronedarone.

Check this interaction

Prucalopride

Unknown severity

DB06480

The serum concentration of Prucalopride can be increased when it is combined with Dronedarone.

Check this interaction

Silodosin

Unknown severity

DB06207

The excretion of Silodosin can be decreased when combined with Dronedarone.

Check this interaction

Topotecan

Unknown severity

DB01030

The serum concentration of Topotecan can be increased when it is combined with Dronedarone.

Check this interaction

Ceritinib

Moderate

DB09063

Dronedarone may increase the bradycardic activities of Ceritinib.

Check this interaction

Valsartan

Moderate

DB00177

Dronedarone may decrease the antihypertensive activities of Valsartan.

Check this interaction

Ramipril

Moderate

DB00178

Dronedarone may decrease the antihypertensive activities of Ramipril.

Check this interaction

Remikiren

Moderate

DB00212

Dronedarone may decrease the antihypertensive activities of Remikiren.

Check this interaction

Torasemide

Moderate

DB00214

Dronedarone may decrease the antihypertensive activities of Torasemide.

Check this interaction

Guanadrel

Moderate

DB00226

Dronedarone may decrease the antihypertensive activities of Guanadrel.

Check this interaction

Olmesartan

Moderate

DB00275

Dronedarone may decrease the antihypertensive activities of Olmesartan.

Check this interaction

Chlorthalidone

Moderate

DB00310

Dronedarone may decrease the antihypertensive activities of Chlorthalidone.

Check this interaction

Nitroprusside

Moderate

DB00325

Dronedarone may decrease the antihypertensive activities of Nitroprusside.

Check this interaction

Minoxidil

Moderate

DB00350

Dronedarone may decrease the antihypertensive activities of Minoxidil.

Check this interaction

Fosinopril

Moderate

DB00492

Dronedarone may decrease the antihypertensive activities of Fosinopril.

Check this interaction

Trandolapril

Moderate

DB00519

Dronedarone may decrease the antihypertensive activities of Trandolapril.

Check this interaction

Metolazone

Moderate

DB00524

Dronedarone may decrease the antihypertensive activities of Metolazone.

Check this interaction

Benazepril

Moderate

DB00542

Dronedarone may decrease the antihypertensive activities of Benazepril.

Check this interaction

Cyclothiazide

Moderate

DB00606

Dronedarone may decrease the antihypertensive activities of Cyclothiazide.

Check this interaction

Candoxatril

Moderate

DB00616

Dronedarone may decrease the antihypertensive activities of Candoxatril.

Check this interaction

Mecamylamine

Moderate

DB00657

Dronedarone may decrease the antihypertensive activities of Mecamylamine.

Check this interaction

Lisinopril

Moderate

DB00722

Dronedarone may decrease the antihypertensive activities of Lisinopril.

Check this interaction

Nitroglycerin

Moderate

DB00727

Dronedarone may decrease the antihypertensive activities of Nitroglycerin.

Check this interaction

Metyrosine

Moderate

DB00765

Dronedarone may decrease the antihypertensive activities of Metyrosine.

Check this interaction

Hydroflumethiazide

Moderate

DB00774

Dronedarone may decrease the antihypertensive activities of Hydroflumethiazide.

Check this interaction

Cryptenamine

Moderate

DB00785

Dronedarone may decrease the antihypertensive activities of Cryptenamine.

Check this interaction

Perindopril

Moderate

DB00790

Dronedarone may decrease the antihypertensive activities of Perindopril.

Check this interaction

Candesartan cilexetil

Moderate

DB00796

Dronedarone may decrease the antihypertensive activities of Candesartan cilexetil.

Check this interaction

Fenoldopam

Moderate

DB00800

Dronedarone may decrease the antihypertensive activities of Fenoldopam.

Check this interaction

Eprosartan

Moderate

DB00876

Dronedarone may decrease the antihypertensive activities of Eprosartan.

Check this interaction

Chlorothiazide

Moderate

DB00880

Dronedarone may decrease the antihypertensive activities of Chlorothiazide.

Check this interaction

Telmisartan

Moderate

DB00966

Dronedarone may decrease the antihypertensive activities of Telmisartan.

Check this interaction

Trichlormethiazide

Moderate

DB01021

Dronedarone may decrease the antihypertensive activities of Trichlormethiazide.

Check this interaction

Deserpidine

Moderate

DB01089

Dronedarone may decrease the antihypertensive activities of Deserpidine.

Check this interaction

Pentolinium

Moderate

DB01090

Dronedarone may decrease the antihypertensive activities of Pentolinium.

Check this interaction

Trimethaphan

Moderate

DB01116

Dronedarone may decrease the antihypertensive activities of Trimethaphan.

Check this interaction

Diazoxide

Moderate

DB01119

The metabolism of Diazoxide can be decreased when combined with Dronedarone.

Check this interaction

Epoprostenol

Moderate

DB01240

Dronedarone may decrease the antihypertensive activities of Epoprostenol.

Check this interaction

Cilazapril

Moderate

DB01340

Dronedarone may decrease the antihypertensive activities of Cilazapril.

Check this interaction

Saprisartan

Moderate

DB01347

Dronedarone may decrease the antihypertensive activities of Saprisartan.

Check this interaction

Spirapril

Moderate

DB01348

Dronedarone may decrease the antihypertensive activities of Spirapril.

Check this interaction

Showing 50 of 1714 interactions

Food & lifestyle interactions

Avoid Grapefruit

Avoid grapefruit products. Co-administration with grapefruit may increase drug concentrations by 3-fold.

Advice

Avoid St. John's Wort. This herb induces CYP3A4 and may increase the serum concentration of dronedarone.

Take With Food

Take with food. Food, especially high-fat food, increases drug absorption.

Toxicity & overdose

In an acute toxicity study, the oral LD₅₀ in rat was >2,000 mg/kg.
[L8687]

In oral studies, dronedarone showed a limited potential for toxicity in humans in acute overdose situations.
[L8684]
However, it is recommended that the patient's cardiac rhythm and blood pressure is monitored in the event of overdose. Symptomatic and supportive treatments should be initiated.
[L8699]

How it works

Mechanism of action

Atrial fibrillation is the most common type of arrhythmia that is caused by abnormal electrical activity in the atria. In atrial fibrillation, tachyarrhythmia, or fast heart rate, can either be paroxysmal (less than 7 days) or persistent (more than 7 days). Atrial fibrillation causes turbulent and abnormal blood flow through the heart chambers, leading to decreased the effectiveness of the heart to pump blood and an increased likelihood of thrombus formation within the atria which can ultimately dislodge and cause a stroke.[L8980]

Dronedarone achieves heart rate and rhythm control in atrial fibrillation. In vitro, dronedarone decreased the maximum rate of the rise of an action potential in a concentration- and frequency-dependent manner.[A186071] Cardiac action potentials are generated by ionic currents of multiple voltage-gated ion channels, including potassium, sodium, and calcium channels.[A187129] Dronedarone is a multichannel blocker that meets the criteria of all four Vaughan Williams antiarrhythmic drug classes[A34604] but the contribution of each of these activities to the drug's antiarrhythmic effect is unknown.[L8699] Dronedarone inhibits rapid Na+ currents rate-dependently (class Ib), non-competitively antagonizes α– and β-adrenergic receptors (class II), blocks K+ outward currents (class III) and blocks slow Ca2+ inward currents (class IV).[A34604] More specifically, it decreases delayed-rectifier K+ current (IKr), slowly activating delayed-rectifier K+ current (IKs), inward rectifier potassium current (IK1), peak Na+ current (INa) and L-type Ca2+ current (ICa (L)).[A186071][A186077] Dronedarone ultimately increases refractory periods, decelerates cardiac conduction, and prolongs cardiac action potential and refractory periods.[A34604][L8684]

Pharmacodynamics

Dronedarone is an antiarrhythmic agent that restores normal sinus rhythm and reduces heart rate in atrial fibrillation. In another model, it prevents ventricular tachycardia and ventricular fibrillation.[L8684] Dronedarone moderately prolongs the QTc interval by about 10 ms on average.[L8699] Dronedarone decreases arterial blood pressure and reduces oxygen consumption. It reduces myocardial contractility with no change in left ventricular ejection fraction. Dronedarone vasodilates coronary arteries through activation of the nitric oxide pathway.[L8684] In clinical studies, dronedarone reduced incidence of hospitalizations for acute coronary syndromes and reduced incidence of stroke.[A186077] Dronedarone exhibits antiadrenergic effects by reducing alpha-adrenergic blood pressure response to epinephrine and beta 1 and beta 2 responses to isoproterenol.[L8684]

Dronedarone was shown to inhibit triiodothyronine (T3) signalling by binding to TRα1 but much less so to TRβ1.[A187138] The treatment of dronedarone in patients with severe heart failure and left ventricular systolic dysfunction was associated with increased early mortality related to the worsening of heart failure.[A186080] In animal studies, the use of dronedarone at doses equivalent to the recommended human doses was associated with fetal harm. In clinical studies and postmarketing reports, dronedarone was shown to cause hepatocellular liver injury and pulmonary toxicities, such as interstitial lung disease, pneumonitis, and pulmonary fibrosis.[L8699] Compared to its related compound [amiodarone], dronedarone has a faster onset and offset of actions with a shorter elimination half-life and low tissue accumulation.[A34604,T28]

Pharmacokinetics

How the body processes this drug — absorption, distribution, metabolism, and elimination

Absorption

Dronedarone is well absorbed after oral administration (>70%).
[A34604]
It displays low systemic bioavailability due to extensive first-pass metabolism. The absolute bioavailability of dronedarone without and with a high-fat meal is 4% and 15%, respectively. The peak plasma concentrations of dronedarone and its main circulating N-debutyl metabolite are reached within 3 to 6 hours after administration with food.

Following repeated administration of 400 mg dronedarone twice daily, the steady-state was reached within 4 to 8 days of initial treatment.

The steady-state Cmax and systemic exposure to the N-debutyl metabolite are similar to that of the parent compound.
[L8699]

Half-life

The elimination half life ranges from 13 to 19 hours.
[L8699]

Protein binding

The in vitro plasma protein binding of dronedarone and its N-debutyl metabolite is 99.7% and 98.5%, respectively. Both mainly bind to albumin and are not capable of saturation.
[A34604]

Volume of distribution

The volume of distribution at steady-state ranges from 1200 to 1400 L following intravenous administration.
[L8699]

Metabolism

Dronedarone predominantly undergoes CYP3A-mediated hepatic metabolism. Initial metabolism of dronedarone involves N-debutylation to form the N-debutyl-dronedarone, which retains 1/10 to 1/3 of pharmacological activity of the parent compound.
[L8699]
N-debutyl-dronedarone can be further metabolized to phenol-dronedarone via O-dealkylation and propanoic acid-dronedarone via oxidative deamination. Dronedarone can also be metabolized by CYP2D6 to form benzofuran-hydroxyl-dronedarone.

Other detectable metabolites include C-dealkyl-dronedarone and dibutylamine-hydroxyl-dronedarone, along with other minor downstream metabolites with undetermined chemical structures.
[A186110]

Route of elimination

Following oral administration, about 84% of the labeled dose is excreted in feces and 6% is excreted in urine, mainly as metabolites. Unchanged parent compound and the N-debutyl metabolite accounted for less than 15% of the total radioactivity in the plasma.
[L8699]

Clearance

Following intravenous administration, the clearance ranged from 130 to 150 L/h.
[L8699]

Drug targets(25)

Proteins and enzymes this drug interacts with in the body

Alpha-1A adrenergic receptor

BE0000501

ADRA1A

antagonist

Specific functionalpha1-adrenergic receptor activity

Cellular location

Nucleus membrane

General function & pharmacology

This alpha-adrenergic receptor mediates its action by association with G proteins that activate a phosphatidylinositol-calcium second messenger system. Its effect is mediated by G(q) and G(11) proteins. Nuclear ADRA1A-ADRA1B heterooligomers regulate phenylephrine(PE)-stimulated ERK signaling in cardiac myocytes

Alpha-1B adrenergic receptor

BE0000575

ADRA1B

antagonist

Specific functionalpha1-adrenergic receptor activity

Cellular location

Nucleus membrane

General function & pharmacology

Alpha-1D adrenergic receptor

BE0000715

ADRA1D

antagonist

Specific functionalpha1-adrenergic receptor activity

Cellular location

Cell membrane

General function & pharmacology

This alpha-adrenergic receptor mediates its effect through the influx of extracellular calcium

Alpha-2A adrenergic receptor

BE0000289

ADRA2A

antagonist

Specific functionalpha-1B adrenergic receptor binding

Cellular location

Cell membrane

General function & pharmacology

Alpha-2 adrenergic receptors mediate the catecholamine-induced inhibition of adenylate cyclase through the action of G proteins. The rank order of potency for agonists of this receptor is oxymetazoline > clonidine > epinephrine > norepinephrine > phenylephrine > dopamine > p-synephrine > p-tyramine > serotonin = p-octopamine. For antagonists, the rank order is yohimbine > phentolamine = mianserine > chlorpromazine = spiperone = prazosin > propanolol > alprenolol = pindolol

Alpha-2B adrenergic receptor

BE0000572

ADRA2B

antagonist

Specific functionalpha2-adrenergic receptor activity

Cellular location

Cell membrane

General function & pharmacology

Alpha-2 adrenergic receptors mediate the catecholamine-induced inhibition of adenylate cyclase through the action of G proteins. The rank order of potency for agonists of this receptor is clonidine > norepinephrine > epinephrine = oxymetazoline > dopamine > p-tyramine = phenylephrine > serotonin > p-synephrine / p-octopamine. For antagonists, the rank order is yohimbine > chlorpromazine > phentolamine > mianserine > spiperone > prazosin > alprenolol > propanolol > pindolol

Metabolizing enzymes(4)

Enzymes involved in drug metabolism — important for understanding drug interactions

Enzyme activity key

substrate

inhibitor

inducer

CYP3A5Cytochrome P450 3A5

substrate

inhibitor

CYP2J2Cytochrome P450 2J2

inhibitor

CYP2D6Cytochrome P450 2D6

substrate

inhibitor

CYP3A4Cytochrome P450 3A4

substrate

inhibitor

Transporters(6)

Proteins that transport this drug across cell membranes

ATP-dependent translocase ABCB1

BE0001032

ABCB1

inhibitor

Specific functionABC-type xenobiotic transporter activity

Cellular location

Cell membrane

General function & pharmacology

Translocates drugs and phospholipids across the membrane .
PMID:2897240 PMID:35970996 PMID:8898203 PMID:9038218 PMID:35507548

Catalyzes the flop of phospholipids from the cytoplasmic to the exoplasmic leaflet of the apical membrane. Participates mainly to the flop of phosphatidylcholine, phosphatidylethanolamine, beta-D-glucosylceramides and sphingomyelins .
PMID:8898203
Energy-dependent efflux pump responsible for decreased drug accumulation in multidrug-resistant cells PMID:2897240 PMID:35970996 PMID:9038218

Solute carrier family 22 member 2

BE0003647

SLC22A2

inhibitor

Specific functionacetylcholine transmembrane transporter activity

Cellular location

Basolateral cell membrane

General function & pharmacology

Electrogenic voltage-dependent transporter that mediates the transport of a variety of organic cations such as endogenous bioactive amines, cationic drugs and xenobiotics .
PMID:9260930 PMID:9687576
Functions as a Na(+)-independent, bidirectional uniporter .
PMID:21128598 PMID:9687576
Cation cellular uptake or release is driven by the electrochemical potential, i.e. membrane potential and concentration gradient .
PMID:15212162 PMID:9260930 PMID:9687576

However, may also engage electroneutral cation exchange when saturating concentrations of cation substrates are reached (By similarity). Predominantly expressed at the basolateral membrane of hepatocytes and proximal tubules and involved in the uptake and disposition of cationic compounds by hepatic and renal clearance from the blood flow .
PMID:15783073
Implicated in monoamine neurotransmitters uptake such as histamine, dopamine, adrenaline/epinephrine, noradrenaline/norepinephrine, serotonin and tyramine, thereby supporting a physiological role in the central nervous system by regulating interstitial concentrations of neurotransmitters .
PMID:16581093 PMID:17460754 PMID:9687576

Also capable of transporting dopaminergic neuromodulators cyclo(his-pro), salsolinol and N-methyl-salsolinol, thereby involved in the maintenance of dopaminergic cell integrity in the central nervous system .
PMID:17460754
Mediates the bidirectional transport of acetylcholine (ACh) at the apical membrane of ciliated cell in airway epithelium, thereby playing a role in luminal release of ACh from bronchial epithelium .
PMID:15817714
Also transports guanidine and endogenous monoamines such as vitamin B1/thiamine, creatinine and N-1-methylnicotinamide (NMN) .
PMID:12089365 PMID:15212162 PMID:17072098 PMID:24961373 PMID:9260930

Mediates the uptake and efflux of quaternary ammonium compound choline .
PMID:9260930
Mediates the bidirectional transport of polyamine agmatine and the uptake of polyamines putrescine and spermidine .
PMID:12538837 PMID:21128598
Able to transport non-amine endogenous compounds such as prostaglandin E2 (PGE2) and prostaglandin F2-alpha (PGF2-alpha) .
PMID:11907186
Also involved in the uptake of xenobiotic 4-(4-(dimethylamino)styryl)-N-methylpyridinium (ASP) .
PMID:12395288 PMID:16394027
May contribute to regulate the transport of organic compounds in testis across the blood-testis-barrier (Probable)

Solute carrier family 22 member 1

BE0003648

SLC22A1

inhibitor

Specific function(R)-carnitine transmembrane transporter activity

Cellular location

Basolateral cell membrane

General function & pharmacology

Electrogenic voltage-dependent transporter that mediates the transport of a variety of organic cations such as endogenous bioactive amines, cationic drugs and xenobiotics .
PMID:11388889 PMID:11408531 PMID:12439218 PMID:12719534 PMID:15389554 PMID:16263091 PMID:16272756 PMID:16581093 PMID:19536068 PMID:21128598 PMID:23680637 PMID:24961373 PMID:34040533 PMID:9187257 PMID:9260930 PMID:9655880

Functions as a pH- and Na(+)-independent, bidirectional transporter (By similarity). Cation cellular uptake or release is driven by the electrochemical potential (i.e. membrane potential and concentration gradient) and substrate selectivity (By similarity). Hydrophobicity is a major requirement for recognition in polyvalent substrates and inhibitors (By similarity).

Primarily expressed at the basolateral membrane of hepatocytes and proximal tubules and involved in the uptake and disposition of cationic compounds by hepatic and renal clearance from the blood flow (By similarity). Most likely functions as an uptake carrier in enterocytes contributing to the intestinal elimination of organic cations from the systemic circulation .
PMID:16263091
Transports endogenous monoamines such as N-1-methylnicotinamide (NMN), guanidine, histamine, neurotransmitters dopamine, serotonin and adrenaline .
PMID:12439218 PMID:24961373 PMID:35469921 PMID:9260930

Also transports natural polyamines such as spermidine, agmatine and putrescine at low affinity, but relatively high turnover .
PMID:21128598
Involved in the hepatic uptake of vitamin B1/thiamine, hence regulating hepatic lipid and energy metabolism .
PMID:24961373
Mediates the bidirectional transport of acetylcholine (ACh) at the apical membrane of ciliated cell in airway epithelium, thereby playing a role in luminal release of ACh from bronchial epithelium .
PMID:15817714
Transports dopaminergic neuromodulators cyclo(his-pro) and salsolinol with lower efficency .
PMID:17460754
Also capable of transporting non-amine endogenous compounds such as prostaglandin E2 (PGE2) and prostaglandin F2-alpha (PGF2-alpha) .
PMID:11907186
May contribute to the transport of cationic compounds in testes across the blood-testis-barrier (Probable). Also involved in the uptake of xenobiotics tributylmethylammonium (TBuMA), quinidine, N-methyl-quinine (NMQ), N-methyl-quinidine (NMQD) N-(4,4-azo-n-pentyl)-quinuclidine (APQ), azidoprocainamide methoiodide (AMP), N-(4,4-azo-n-pentyl)-21-deoxyajmalinium (APDA) and 4-(4-(dimethylamino)styryl)-N-methylpyridinium (ASP) PMID:11408531 PMID:15389554 PMID:35469921 PMID:9260930

Solute carrier organic anion transporter family member 1B1

BE0001004

SLCO1B1

inhibitor

Specific functionbile acid transmembrane transporter activity

Cellular location

Basolateral cell membrane

General function & pharmacology

Mediates the Na(+)-independent uptake of organic anions .
PMID:10358072 PMID:15159445 PMID:17412826

Shows broad substrate specificity, can transport both organic anions such as bile acid taurocholate (cholyltaurine) and conjugated steroids (dehydroepiandrosterone 3-sulfate, 17-beta-glucuronosyl estradiol, and estrone 3-sulfate), as well as eicosanoids (prostaglandin E2, thromboxane B2, leukotriene C4, and leukotriene E4), and thyroid hormones (T4/L-thyroxine, and T3/3,3',5'-triiodo-L-thyronine) .
PMID:10358072 PMID:10601278 PMID:10873595 PMID:11159893 PMID:12196548 PMID:12568656 PMID:15159445 PMID:15970799 PMID:16627748 PMID:17412826 PMID:19129463 PMID:26979622

Can take up bilirubin glucuronides from plasma into the liver, contributing to the detoxification-enhancing liver-blood shuttling loop .
PMID:22232210
Involved in the clearance of endogenous and exogenous substrates from the liver .
PMID:10358072 PMID:10601278
Transports coproporphyrin I and III, by-products of heme synthesis, and may be involved in their hepatic disposition .
PMID:26383540
May contribute to regulate the transport of organic compounds in testes across the blood-testis-barrier (Probable). Can transport HMG-CoA reductase inhibitors (also known as statins), such as pravastatin and pitavastatin, a clinically important class of hypolipidemic drugs .
PMID:10601278 PMID:15159445 PMID:15970799

May play an important role in plasma and tissue distribution of the structurally diverse chemotherapeutic drug methotrexate .
PMID:23243220
May also transport antihypertension agents, such as the angiotensin-converting enzyme (ACE) inhibitor prodrug enalapril, and the highly selective angiotensin II AT1-receptor antagonist valsartan, in the liver .
PMID:16624871 PMID:16627748
Shows a pH-sensitive substrate specificity towards prostaglandin E2 and T4 which may be ascribed to the protonation state of the binding site and leads to a stimulation of substrate transport in an acidic microenvironment .
PMID:19129463
Hydrogencarbonate/HCO3(-) acts as the probable counteranion that exchanges for organic anions PMID:19129463

Solute carrier organic anion transporter family member 1B3

BE0003659

SLCO1B3

inhibitor

Specific functionbile acid transmembrane transporter activity

Cellular location

Basolateral cell membrane

General function & pharmacology

Mediates the Na(+)-independent uptake of organic anions .
PMID:10779507 PMID:15159445 PMID:17412826

Shows broad substrate specificity, can transport both organic anions such as bile acid taurocholate (cholyltaurine) and conjugated steroids (17-beta-glucuronosyl estradiol, dehydroepiandrosterone sulfate (DHEAS), and estrone 3-sulfate), as well as eicosanoid leukotriene C4, prostaglandin E2 and L-thyroxine (T4) .
PMID:10779507 PMID:11159893 PMID:12568656 PMID:15159445 PMID:17412826 PMID:19129463

Hydrogencarbonate/HCO3(-) acts as the probable counteranion that exchanges for organic anions .
PMID:19129463
Shows a pH-sensitive substrate specificity towards sulfated steroids, taurocholate and T4 which may be ascribed to the protonation state of the binding site and leads to a stimulation of substrate transport in an acidic microenvironment .
PMID:19129463
Involved in the clearance of bile acids and organic anions from the liver .
PMID:22232210
Can take up bilirubin glucuronides from plasma into the liver, contributing to the detoxification-enhancing liver-blood shuttling loop .
PMID:22232210
Transports coproporphyrin I and III, by-products of heme synthesis, and may be involved in their hepatic disposition .
PMID:26383540
May contribute to regulate the transport of organic compounds in testes across the blood-testis-barrier (Probable). Can transport HMG-CoA reductase inhibitors (also known as statins) such as pitavastatin, a clinically important class of hypolipidemic drugs .
PMID:15159445
May play an important role in plasma and tissue distribution of the structurally diverse chemotherapeutic drugs methotrexate and paclitaxel .
PMID:23243220
May also transport antihypertension agents, such as the angiotensin-converting enzyme (ACE) inhibitor prodrug enalapril, and the highly selective angiotensin II AT1-receptor antagonist valsartan, in the liver PMID:16624871 PMID:16627748

Organic anion transporter 3

BE0003645

SLC22A8

inhibitor

Specific functionorganic anion transmembrane transporter activity

Cellular location

Basolateral cell membrane

General function & pharmacology

Functions as an organic anion/dicarboxylate exchanger that couples organic anion uptake indirectly to the sodium gradient .
PMID:14586168 PMID:15644426 PMID:15846473 PMID:16455804 PMID:31553721

Transports organic anions such as estrone 3-sulfate (E1S) and urate in exchange for dicarboxylates such as glutarate or ketoglutarate (2-oxoglutarate) .
PMID:14586168 PMID:15846473 PMID:15864504 PMID:22108572 PMID:23832370

Plays an important role in the excretion of endogenous and exogenous organic anions, especially from the kidney and the brain .
PMID:11306713 PMID:14586168 PMID:15846473

E1S transport is pH- and chloride-dependent and may also involve E1S/cGMP exchange .
PMID:26377792
Responsible for the transport of prostaglandin E2 (PGE2) and prostaglandin F2(alpha) (PGF2(alpha)) in the basolateral side of the renal tubule .
PMID:11907186
Involved in the transport of neuroactive tryptophan metabolites kynurenate and xanthurenate .
PMID:22108572 PMID:23832370
Functions as a biopterin transporters involved in the uptake and the secretion of coenzymes tetrahydrobiopterin (BH4), dihydrobiopterin (BH2) and sepiapterin to urine, thereby determining baseline levels of blood biopterins .
PMID:28534121
May be involved in the basolateral transport of steviol, a metabolite of the popular sugar substitute stevioside .
PMID:15644426
May participate in the detoxification/ renal excretion of drugs and xenobiotics, such as the histamine H(2)-receptor antagonists fexofenadine and cimetidine, the antibiotic benzylpenicillin (PCG), the anionic herbicide 2,4-dichloro-phenoxyacetate (2,4-D), the diagnostic agent p-aminohippurate (PAH), the antiviral acyclovir (ACV), and the mycotoxin ochratoxin (OTA), by transporting these exogenous organic anions across the cell membrane in exchange for dicarboxylates such as 2-oxoglutarate .
PMID:11669456 PMID:15846473 PMID:16455804

Contributes to the renal uptake of potent uremic toxins (indoxyl sulfate (IS), indole acetate (IA), hippurate/N-benzoylglycine (HA) and 3-carboxy-4-methyl-5-propyl-2-furanpropionate (CMPF)), pravastatin, PCG, E1S and dehydroepiandrosterone sulfate (DHEAS), and is partly involved in the renal uptake of temocaprilat (an angiotensin-converting enzyme (ACE) inhibitor) .
PMID:14675047
May contribute to the release of cortisol in the adrenals .
PMID:15864504
Involved in one of the detoxification systems on the choroid plexus (CP), removes substrates such as E1S or taurocholate (TC), PCG, 2,4-D and PAH, from the cerebrospinal fluid (CSF) to the blood for eventual excretion in urine and bile (By similarity). Also contributes to the uptake of several other organic compounds such as the prostanoids prostaglandin E(2) and prostaglandin F(2-alpha), L-carnitine, and the therapeutic drugs allopurinol, 6-mercaptopurine (6-MP) and 5-fluorouracil (5-FU) (By similarity). Mediates the transport of PAH, PCG, and the statins pravastatin and pitavastatin, from the cerebrum into the blood circulation across the blood-brain barrier (BBB).

In summary, plays a role in the efflux of drugs and xenobiotics, helping reduce their undesired toxicological effects on the body (By similarity)

Carriers(1)

Proteins that carry this drug through the body

Albumin

BE0000530

ALB

binder

Specific functionantioxidant activity

Cellular location

Secreted

General function & pharmacology

Binds water, Ca(2+), Na(+), K(+), fatty acids, hormones, bilirubin and drugs (Probable). Its main function is the regulation of the colloidal osmotic pressure of blood (Probable). Major zinc transporter in plasma, typically binds about 80% of all plasma zinc .
PMID:19021548
Major calcium and magnesium transporter in plasma, binds approximately 45% of circulating calcium and magnesium in plasma (By similarity).

Potentially has more than two calcium-binding sites and might additionally bind calcium in a non-specific manner (By similarity). The shared binding site between zinc and calcium at residue Asp-273 suggests a crosstalk between zinc and calcium transport in the blood (By similarity). The rank order of affinity is zinc > calcium > magnesium (By similarity).

Binds to the bacterial siderophore enterobactin and inhibits enterobactin-mediated iron uptake of E.coli from ferric transferrin, and may thereby limit the utilization of iron and growth of enteric bacteria such as E.coli .
PMID:6234017
Does not prevent iron uptake by the bacterial siderophore aerobactin PMID:6234017

Scientific references(7)

Schweizer P.A., Becker R., Katus H.A., Thomas D.

Dronedarone: current evidence for its safety and efficacy in the management of atrial fibrillation.

Drug Des Devel Therapeutics

2011 Jan 65:27-39. doi: 10.2147/DDDT.S10315

PMID: 21267357 DOI: 10.2147/DDDT.S10315

Patel P.D., Bhuriya R., Patel D.D., Arora B.L., Singh P.P., Arora R.R.

Dronedarone for atrial fibrillation: a new therapeutic agent.

Vasc Health Risk Manag

20095:635-42. doi: 10.2147/vhrm.s6185. Epub 2009 Aug 6

PMID: 19688104 DOI: 10.2147/vhrm.s6185

Heijman J., Heusch G., Dobrev D.

Pleiotropic effects of antiarrhythmic agents: dronedarone in the treatment of atrial fibrillation.

Clinical Medicine Insights Cardiology

2013 Aug 117:127-40. doi: 10.4137/CMC.S8445. eCollection 2013

PMID: 23997577 DOI: 10.4137/CMC.S8445

Kober L., Torp-Pedersen C., McMurray J.J., Gotzsche O., Levy S., Crijns H., Amlie J., Carlsen J.

Increased mortality after dronedarone therapy for severe heart failure.

New England Journal of Medicine

2008 Jun 19358(25):2678-87. doi: 10.1056/NEJMoa0800456

PMID: 18565860 DOI: 10.1056/NEJMoa0800456

Klieber S., Arabeyre-Fabre C., Moliner P., Marti E., Mandray M., Ngo R., Ollier C., Brun P., Fabre G.

Identification of metabolic pathways and enzyme systems involved in the in vitro human hepatic metabolism of dronedarone, a potent new oral antiarrhythmic drug.

Pharmacology Research Perspect

2014 Jun2(3):e00044. doi: 10.1002/prp2.44. Epub 2014 Apr 22

PMID: 25505590 DOI: 10.1002/prp2.44

Rahm A.K., Lugenbiel P., Schweizer P.A., Katus H.A., Thomas D.

Role of ion channels in heart failure and channelopathies.

Biophys Review

2018 Aug10(4):1097-1106. doi: 10.1007/s12551-018-0442-3. Epub 2018 Jul 17

PMID: 30019205 DOI: 10.1007/s12551-018-0442-3

Van Beeren H.C., Jong W.M., Kaptein E., Visser T.J., Bakker O., Wiersinga W.M.

Dronerarone acts as a selective inhibitor of 3,5,3'-triiodothyronine binding to thyroid hormone receptor-alpha1: in vitro and in vivo evidence.

Endocrinology

2003 Feb144(2):552-8. doi: 10.1210/en.2002-220604

PMID: 12538616 DOI: 10.1210/en.2002-220604

ATC classification(1 code)

ATC C01BD07

Affected organisms(1)

Humans and other mammals

Salt forms(1)

Dronedarone hydrochloride(DBSALT000061)

Experimental properties(3)

External resources(2)

RxList Drugs.com

Commercial products(9)

Chemical identifiers

CAS, UNII, InChI Key and database cross-references

Show

Linked compound data from DrugBank Open Data (CC BY-NC 4.0)

Dronedarone

DB04855

CAS number

141626-36-0

UNII (FDA)

JQZ1L091Y2

InChI Key (molecular fingerprint)

ZQTNQVWKHCQYLQ-UHFFFAOYSA-N

Additional database identifiers

Drugs Product Database (DPD)

20511

ChEBI

50659

PubChem Compound

208898

PubChem Substance

175426865

KEGG Drug

D02537

ChemSpider

180996

BindingDB

50151864

PharmGKB

PA153619853

Wikipedia

Dronedarone

ChEMBL

CHEMBL184412

ZINC

ZINC000049933061

RxCUI

233698

HUGO Gene Nomenclature Committee (HGNC)

HGNC:277

GenAtlas

ADRA1A

GeneCards

ADRA1A

GenBank Gene Database

D25235

GenBank Protein Database

433201

IUPHAR

Guide to Pharmacology

UniProtKB

P35348

UniProt Accession

ADA1A_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:278

GenAtlas

ADRA1B

GeneCards

ADRA1B

GenBank Gene Database

M99589

IUPHAR

Guide to Pharmacology

UniProtKB

P35368

UniProt Accession

ADA1B_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:280

GenAtlas

ADRA1D

GeneCards

ADRA1D

GenBank Gene Database

M76446

GenBank Protein Database

177807

IUPHAR

Guide to Pharmacology

UniProtKB

P25100

UniProt Accession

ADA1D_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:281

GenAtlas

ADRA2A

GeneCards

ADRA2A

GenBank Gene Database

M23533

GenBank Protein Database

178196

IUPHAR

Guide to Pharmacology

UniProtKB

P08913

UniProt Accession

ADA2A_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:282

GenAtlas

ADRA2B

GeneCards

ADRA2B

GenBank Gene Database

M34041

GenBank Protein Database

178198

IUPHAR

Guide to Pharmacology

UniProtKB

P18089

UniProt Accession

ADA2B_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:283

GenAtlas

ADRA2C

GeneCards

ADRA2C

GenBank Gene Database

J03853

GenBank Protein Database

178194

IUPHAR

Guide to Pharmacology

UniProtKB

P18825

UniProt Accession

ADA2C_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:6251

GenAtlas

KCNH2

GeneCards

KCNH2

GenBank Gene Database

U04270

GenBank Protein Database

487738

IUPHAR

572

Guide to Pharmacology

572

UniProtKB

Q12809

UniProt Accession

KCNH2_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:1390

GenAtlas

CACNA1C

GeneCards

CACNA1C

GenBank Gene Database

M92270

IUPHAR

529

Guide to Pharmacology

529

UniProtKB

Q13936

UniProt Accession

CAC1C_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:1391

GenAtlas

CACNA1D

GeneCards

CACNA1D

GenBank Gene Database

M76558

GenBank Protein Database

179764

IUPHAR

530

Guide to Pharmacology

530

UniProtKB

Q01668

UniProt Accession

CAC1D_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:1393

GenAtlas

CACNA1F

GeneCards

CACNA1F

GenBank Gene Database

AJ006216

GenBank Protein Database

3183953

IUPHAR

531

Guide to Pharmacology

531

UniProtKB

O60840

UniProt Accession

CAC1F_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:1397

GenAtlas

CACNA1S

GeneCards

CACNA1S

GenBank Gene Database

U30707

GenBank Protein Database

1698403

IUPHAR

528

Guide to Pharmacology

528

UniProtKB

Q13698

UniProt Accession

CAC1S_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:1401

GenAtlas

CACNB1

GeneCards

CACNB1

GenBank Gene Database

M92303

GenBank Protein Database

179806

UniProtKB

Q02641

UniProt Accession

CACB1_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:1402

GenAtlas

CACNB2

GeneCards

CACNB2

GenBank Gene Database

S60415

GenBank Protein Database

300417

UniProtKB

Q08289

UniProt Accession

CACB2_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:1403

GenAtlas

CACNB3

GeneCards

CACNB3

GenBank Gene Database

X76555

GenBank Protein Database

435135

UniProtKB

P54284

UniProt Accession

CACB3_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:1404

GenAtlas

CACNB4

GeneCards

CACNB4

GenBank Gene Database

U95020

GenBank Protein Database

2058727

UniProtKB

O00305

UniProt Accession

CACB4_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:6277

GenAtlas

KCNK2

GeneCards

KCNK2

GenBank Gene Database

AF129399

GenBank Protein Database

5712621

IUPHAR

514

Guide to Pharmacology

514

UniProtKB

O95069

UniProt Accession

KCNK2_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:10593

GenAtlas

SCN5A

GeneCards

SCN5A

GenBank Gene Database

M77235

GenBank Protein Database

184039

IUPHAR

582

Guide to Pharmacology

582

UniProtKB

Q14524

UniProt Accession

SCN5A_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:6264

GenAtlas

KCNJ3

GeneCards

KCNJ3

GenBank Gene Database

U39196

GenBank Protein Database

1055028

IUPHAR

434

Guide to Pharmacology

434

UniProtKB

P48549

UniProt Accession

KCNJ3_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:6294

GenAtlas

KCNQ1

GeneCards

KCNQ1

GenBank Gene Database

AF000571

GenBank Protein Database

2465531

IUPHAR

560

Guide to Pharmacology

560

UniProtKB

P51787

UniProt Accession

KCNQ1_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:6258

GenAtlas

KCNJ12

GeneCards

KCNJ12

GenBank Gene Database

L36069

GenBank Protein Database

567019

IUPHAR

431

Guide to Pharmacology

431

UniProtKB

Q14500

UniProt Accession

KCJ12_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:6260

GeneCards

KCNJ14

Guide to Pharmacology

433

UniProtKB

Q9UNX9

UniProt Accession

KCJ14_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:6263

GeneCards

KCNJ2

UniProtKB

P63252

UniProt Accession

KCNJ2_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:6265

GeneCards

KCNJ4

Guide to Pharmacology

432

UniProtKB

P48050

UniProt Accession

KCNJ4_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:11068

GenAtlas

SLC8A1

GeneCards

SLC8A1

GenBank Gene Database

M91368

GenBank Protein Database

180673

UniProtKB

P32418

UniProt Accession

NAC1_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:6239

GeneCards

KCND3

GenBank Gene Database

AF048712

GenBank Protein Database

2935434

UniProtKB

Q9UK17

UniProt Accession

KCND3_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:6224

GeneCards

KCNA5

Guide to Pharmacology

542

UniProtKB

P22460

UniProt Accession

KCNA5_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:285

GenAtlas

ADRB1

GeneCards

ADRB1

GenBank Gene Database

J03019

GenBank Protein Database

178200

IUPHAR

Guide to Pharmacology

UniProtKB

P08588

UniProt Accession

ADRB1_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:11796

GenAtlas

THRA

GeneCards

THRA

GenBank Gene Database

X55074

GenBank Protein Database

825639

IUPHAR

588

Guide to Pharmacology

588

UniProtKB

P10827

UniProt Accession

THA_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:2638

GenAtlas

CYP3A5

GeneCards

CYP3A5

GenBank Gene Database

J04813

GenBank Protein Database

181346

Guide to Pharmacology

1338

UniProtKB

P20815

UniProt Accession

CP3A5_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:2634

GeneCards

CYP2J2

GenBank Gene Database

U37143

GenBank Protein Database

18254513

Guide to Pharmacology

1332

UniProtKB

P51589

UniProt Accession

CP2J2_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:2625

GenAtlas

CYP2D6

GeneCards

CYP2D6

GenBank Gene Database

M20403

GenBank Protein Database

181350

Guide to Pharmacology

1329

UniProtKB

P10635

UniProt Accession

CP2D6_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:2637

GenAtlas

CYP3A4

GeneCards

CYP3A4

GenBank Gene Database

M18907

Guide to Pharmacology

1337

UniProtKB

P08684

UniProt Accession

CP3A4_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:399

GenAtlas

ALB

GeneCards

ALB

GenBank Gene Database

V00494

GenBank Protein Database

28590

UniProtKB

P02768

UniProt Accession

ALBU_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:40

GenAtlas

ABCB1

GeneCards

ABCB1

GenBank Gene Database

M14758

GenBank Protein Database

307180

Guide to Pharmacology

768

UniProtKB

P08183

UniProt Accession

MDR1_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:10966

GeneCards

SLC22A2

GenBank Gene Database

X98333

GenBank Protein Database

2281942

Guide to Pharmacology

1020

UniProtKB

O15244

UniProt Accession

S22A2_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:10963

GeneCards

SLC22A1

GenBank Gene Database

X98332

GenBank Protein Database

2511670

Guide to Pharmacology

1019

UniProtKB

O15245

UniProt Accession

S22A1_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:10959

GenAtlas

SLCO1B1

GeneCards

SLCO1B1

GenBank Gene Database

AF060500

GenBank Protein Database

5051630

Guide to Pharmacology

1220

UniProtKB

Q9Y6L6

UniProt Accession

SO1B1_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:10961

GeneCards

SLCO1B3

GenBank Gene Database

AJ251506

GenBank Protein Database

9187497

Guide to Pharmacology

1221

UniProtKB

Q9NPD5

UniProt Accession

SO1B3_HUMAN

HUGO Gene Nomenclature Committee (HGNC)

HGNC:10972

GeneCards

SLC22A8

GenBank Gene Database

AF097491

GenBank Protein Database

4378059

Guide to Pharmacology

1027

UniProtKB

Q8TCC7

UniProt Accession

S22A8_HUMAN

Patent information

3 active patents, 5 expired

8602215

United States

Approved 10 Dec 2013 · Expires 30 Jun 2031

5y 2m

8410167

United States

Approved 2 Apr 2013 · Expires 16 Apr 2029

3 years

9107900

United States

Approved 18 Aug 2015 · Expires 16 Apr 2029

3 years

2294812

Canada

Approved 29 Sept 2009 · Expires 19 Jun 2018

Expired

8318800

United States

Approved 27 Nov 2012 · Expires 19 Jun 2018

Expired

Source: DrugBank · CC BY-NC 4.0. Patent data sourced from national patent offices. Expiry dates may not reflect extensions, regulatory exclusivity periods, or legal challenges.

DrugBank citations

If you use DrugBank data in your research, please cite the following publications:

Knox C., Wilson M., Klinger C.M., et al

DrugBank 6.

0: the DrugBank Knowledgebase for 2024

Nucleic Acids Res. 2024 Jan 552(D1):D1265-D1275

PMID: 37953279

Wishart D.S., Feunang Y.D., Guo A.C., et al

DrugBank 5.

0: a major update to the DrugBank database for 2018

Nucleic Acids Res. 2017 Nov 846(D1):D1074-D1082

PMID: 29126136

Show earlier publications

Law V., Knox C., Djoumbou Y., et al

DrugBank 4.

0: shedding new light on drug metabolism

Nucleic Acids Res. 2014 Jan 142(1):D1091-7

PMID: 24203711

Knox C., Law V., Jewison T., et al

DrugBank 3.

0: a comprehensive resource for 'omics' research on drugs

Nucleic Acids Res. 2011 Jan39(Database issue):D1035-41

PMID: 21059682

Wishart D.S., Knox C., Guo A.C., et al

DrugBank: a knowledgebase for drugs, drug actions and drug targets.

Nucleic Acids Research

2008 Jan36(Database issue):D901-6

PMID: 18048412

Wishart D.S., Knox C., Guo A.C., et al

DrugBank: a comprehensive resource for in silico drug discovery and exploration.

Nucleic Acids Research

2006 Jan 134(Database issue):D668-72

PMID: 16381955

Source: go.drugbank.comCC BY-NC 4.0

Updated about 1 month ago(4 Mar 2026)

Back to medicines

Dronedarone 400mg tablets

Official medicine documents

Safety monitoring data

Yellow Card reports

EudraVigilance

WHO defined daily dose (DDD)

British National Formulary

NICE clinical guidance(3)

Pharmacy stock checkers

Supply & product information

NHS UK identifiers

International identifiers

Browse tools

Key facts

Pharmacokinetics at a glance

Absorption

Half-life

Protein binding

Volume of distribution

Metabolism

Elimination

Clearance

Clinical essentials

Pharmacology

Deep science
36

Chemical identifiers

Dronedarone

Additional database identifiers

Patent information

DrugBank citations

Dronedarone 400mg tablets

Safety & regulatory

Official medicine documents

Safety monitoring data

Yellow Card reports

EudraVigilance

Brand versions and licensed products

NHS reimbursement price

WHO defined daily dose (DDD)

Medicines like this

Prescribing statistics

Guidance (NICE / BNF)

British National Formulary

NICE clinical guidance(3)

Availability, stocks & shortages

Pharmacy stock checkers

Supply & product information

Professional identifiers

NHS UK identifiers

International identifiers

Browse tools

Clinical trials

DrugBank data

Key facts

Pharmacokinetics at a glance

Absorption

Half-life

Protein binding

Volume of distribution

Metabolism

Elimination

Clearance

Clinical essentials

Pharmacology

Deep science36

Chemical identifiers

Dronedarone

Additional database identifiers

Patent information

DrugBank citations

Deep science
36