Atrial fibrillation (main): Difference between revisions
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(Added NOAC dosing table for nonvalvular AF (apixaban, rivaroxaban, dabigatran, edoxaban) with dose reduction criteria, reversal agents, and ED prescribing guidance; added MedicationDose SMW annotations for all 4 NOACs) |
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==Background== | ==Background== | ||
*Chronic and paroxysmal a fib are associated with thrombus formation | [[File:RiskFactors.jpg|thumb|Non-modifiable risk factors (top left box) and modifiable risk factors (bottom left box) for atrial fibrillation. The main sequelae of atrial fibrillation are in the right box.]] | ||
*Chronic and paroxysmal a-fib are associated with thrombus formation | |||
{{Afib background}} | {{Afib background}} | ||
| Line 16: | Line 17: | ||
==Differential Diagnosis== | ==Differential Diagnosis== | ||
{{Tachycardia (narrow) DDX}} | |||
{{Tachycardia (wide) DDX}} | |||
{{Palpitations DDX}} | {{Palpitations DDX}} | ||
== | ==Evaluation== | ||
[[File:Afib.jpg|thumb|Atrial fibrillation at approximately 150 beats per minute]] | |||
[[File:ECG Atrial Fibrillation.jpg|thumb|A 12-lead ECG showing atrial fibrillation at approximately 132 beats per minute.]] | |||
===ED Work-Up=== | ===ED Work-Up=== | ||
*[[ECG]]<ref>2014 AHA/ACC/HRS Guideline for the Management of Patients With Atrial Fibrillation: Executive Summary. J Am Coll Cardiol. 2014;64(21):2246-2280. | *[[ECG]]<ref>2014 AHA/ACC/HRS Guideline for the Management of Patients With Atrial Fibrillation: Executive Summary. J Am Coll Cardiol. 2014;64(21):2246-2280. doi:10.1016/j.jacc.2014.03.021</ref> | ||
*Eval for [[ACS]] only in: | *Eval for [[ACS]] only in: | ||
**Patient with ECG changes suggestive of ischemia, [[hypotension]], [[angina]] | **Patient with ECG changes suggestive of ischemia, [[hypotension]], [[angina]] | ||
**A fib is rarely only manifestation of ACS, although RVR and hypotension can provoke demand ischemia | **A fib is rarely only manifestation of ACS, although RVR and hypotension can provoke demand ischemia | ||
* | *Acute lab studies for all patients: | ||
** | **CBC | ||
**Chem-10 | **Chem-10 | ||
**Coagulation studies (for patients requiring anticoagulation) | |||
*Additional labs (consider based on clinical scenario): | |||
**TSH & free T4 (Afib increased in sublinical [[hyperthyroidism]]) | |||
**BNP | |||
**D-dimer | |||
**Troponin | |||
**Magnesium level | **Magnesium level | ||
** | **[[Digoxin]] level (if appropriate) | ||
*Imaging | |||
**CXR (if concern for heart failure or infection) | |||
**Chest/Abdominal CT (if concern for sepsis) | |||
=== | ===Diagnosis=== | ||
[[File:Afib.jpg|thumb| | [[File:Afib ecg.jpg|thumb|ECG of atrial fibrillation (top) and normal sinus rhythm (bottom). The purple arrow indicates a P wave, which is lost in atrial fibrillation.]] | ||
'' | |||
''Based on one of three ECG patterns:'' | |||
#Typical | #Typical | ||
#*Irregularly, irregular R waves | #*Irregularly, irregular R waves | ||
| Line 38: | Line 56: | ||
#Large fibrillatory waves | #Large fibrillatory waves | ||
#*May look like flutter waves | #*May look like flutter waves | ||
#**Unlike a-flutter, the fibrillatory waves are irregular | #**Unlike a-flutter, the fibrillatory waves are irregular | ||
#Slow, regular A-fib | #Slow, regular A-fib | ||
#*Due to complete AV block with escape rhythm | #*Due to complete AV block with escape rhythm | ||
*Ischemic changes? | *Ischemic changes? | ||
*Rate > 250? (think preexcitation) | *Rate > 250? (think preexcitation) | ||
| Line 46: | Line 64: | ||
==Management== | ==Management== | ||
''See [[atrial fibrillation with RVR]] for emergent treatment'' | ''See [[atrial fibrillation with RVR]] for emergent treatment'' | ||
===Rate vs. Rhythm Control=== | ===Rate vs. Rhythm Control=== | ||
* | *Rhythm control (i.e. [[synchronized cardioversion]]) | ||
**If <48 hours of symptoms, do not need to anticoagulate prior to rhythm control (may perform in ED)<ref>EBQ:48hr Cardioversion for Afib]]</ref> | **Consider in the emergency department for:<ref>EBQ:Ottawa Aggressive ED Cardioversion Protocol</ref> | ||
**If >48 hours of symptoms, | ***Unstable (due to rhythm) | ||
***Younger patients (<65 years old) with new or paroxysmal episode (<48 hours)<ref>Atrial Fibrillation: Would You Prefer a Pill or 150 Joules? Ann Emerg Med. 2015;66:655-657.</ref> | |||
**Procedural anticoagulation status | |||
***If <48 hours of symptoms, do not need to anticoagulate prior to rhythm control (may perform in ED)<ref>EBQ:48hr Cardioversion for Afib]]</ref> | |||
***If >48 hours of symptoms, need have rhythm control as out patient referral (if stable) | |||
**Method: [[Procedural sedation]] and analgesia (e.g. [[fentanyl]] and [[propofol]]). Apply pads in anterior to posterior position. Synchronized electrical cardioversion starting at 150 to 200 J. | |||
*Rate control for all others or cardioversion failure | *Rate control for all others or cardioversion failure | ||
**[[Beta-blocker]] | **General principal - IV medications for immediate rate control followed by PO medications for sustained rate control | ||
**[[Beta-blocker]] | |||
***Metoprolol 5 mg IV q 5 min (max 3 doses) followed by 25-100 mg PO | |||
**[[Calcium channel blocker]] | |||
***Diltiazem 0.25 mg/kg to 0.35 mg/kg IV (20 mg typical starting dose), can follow with 25 mg IV as second dose if needed | |||
***Followed by PO dose 60-120 mg | |||
***If unable to get sustained response with IV push, consider diltiazem gtt | |||
**[[Digoxin]] | |||
***Indicated if patient hypotensive and cannot get AV nodal blockade or if patient has advanced heart failure | |||
***Typical digitizing dose 500 mcg then 250 mcg q4hx 2 for total dose of 1000 mcg | |||
***Requires renal dosing if patient has impaired renal function | |||
**[[Amiodarone]] | |||
***Indicated if patient has hypotension or advanced heart failure, usually second line after digoxin | |||
***Typical dosing 150 mg IV x 10 min then 1 mg/min x 6 hours then 0.5 mg/minx 18 hours | |||
***Amiodarone can convert patient to sinus rhythm. Consider simultaneously starting empiric anticoagulation if high thromboembolism risk, see below | |||
**[[Procainamide]] | |||
***Indicated: Hemodynamically stable with systolic Blood Pressure >100 mmHg, less than 48 hrs onset, Normal Serum Potassium and Serum Magnesium | |||
***Ottawa protocol Method: Procainamide 1 g IV over 60 minutes. Monitor with frequent Blood Pressures, and hold Procainamide if systolic Blood Pressure <100 mmHg. Monitor telemetry for Arrhythmia, QTc Prolongation, QRS Widening and for successful cardioversion. | |||
{{Anticoagulation in atrial fibrillation}} | {{Anticoagulation in atrial fibrillation}} | ||
====NOAC Dosing for Nonvalvular AF==== | |||
''NOACs are preferred over [[warfarin]] for nonvalvular AF (AHA/ACC/HRS 2019, CCS 2020).<ref>January CT, Wann LS, Calkins H, et al. 2019 AHA/ACC/HRS Focused Update of the 2014 AHA/ACC/HRS Guideline for the Management of Patients With Atrial Fibrillation. J Am Coll Cardiol. 2019;74(1):104-132.</ref><ref>Andrade JG, et al. 2020 CCS/CHRS Comprehensive Guidelines for the Management of Atrial Fibrillation. Can J Cardiol. 2020;36(12):1847-1948.</ref> Contraindicated in mechanical heart valves and moderate-severe mitral stenosis.'' | |||
{| class="wikitable" | |||
|- | |||
! Agent !! Standard Dose !! Reduced Dose !! Criteria for Dose Reduction !! Reversal Agent | |||
|- | |||
| [[Apixaban]] (Eliquis) || 5 mg PO BID || 2.5 mg PO BID || Any 2 of: age ≥80, weight ≤60 kg, Cr ≥1.5 || [[Andexanet alfa]] | |||
|- | |||
| [[Rivaroxaban]] (Xarelto) || 20 mg PO daily with evening meal || 15 mg PO daily with evening meal || CrCl 15-50 || [[Andexanet alfa]] | |||
|- | |||
| [[Dabigatran]] (Pradaxa) || 150 mg PO BID || 75 mg PO BID || CrCl 15-30; or CrCl 30-50 + concomitant P-gp inhibitor || [[Idarucizumab]] | |||
|- | |||
| [[Edoxaban]] (Savaysa) || 60 mg PO daily || 30 mg PO daily || CrCl 15-50 or weight ≤60 kg; avoid if CrCl >95 || No specific agent; consider PCC | |||
|} | |||
*'''ED Prescribing''' | |||
**CCS recommends initiating OAC in the ED for at-risk patients prior to discharge | |||
**Obtain CrCl before prescribing (all NOACs require renal dose adjustment) | |||
**Check for drug interactions (P-gp inhibitors, dual CYP3A4/P-gp inhibitors) | |||
**NOACs should NOT be used in: mechanical heart valves, moderate-severe [[mitral stenosis]], severe renal impairment (CrCl <15 for most agents), or [[antiphospholipid syndrome]] | |||
*'''Advantages over [[warfarin]]''' | |||
**No INR monitoring required | |||
**Fewer drug and food interactions | |||
**Rapid onset (1-3 hours) | |||
**Lower rates of intracranial hemorrhage | |||
*'''Reversal''' — see [[Anticoagulant reversal for life-threatening bleeds]] | |||
====CHADS2-VAsc Score==== | ====CHADS2-VAsc Score==== | ||
| Line 62: | Line 132: | ||
| [[CHF]]||1 | | [[CHF]]||1 | ||
|- | |- | ||
| [[ | | [[hypertension]]||1 | ||
|- | |- | ||
| [[DM]]||1 | | [[DM]]||1 | ||
| Line 80: | Line 150: | ||
*Score 0: consider no treatment or [[ASA]] | *Score 0: consider no treatment or [[ASA]] | ||
*Score 1: consider [[warfarin]] or [[ASA]] | *Score 1: consider [[warfarin]] or [[ASA]] | ||
*Score 2-6: consider [[warfarin]] (INR goal = 2-3) | *Score 2-6: consider [[warfarin]] (INR goal = 2-3) | ||
*All patients with significant valvular disease should be on anticoagulation | *All patients with significant valvular disease should be on anticoagulation | ||
| Line 113: | Line 183: | ||
==Disposition== | ==Disposition== | ||
''Similar outcomes for Canadian vs. American strategies, despite lower admission rates in Canada<ref>Rising KL. Home is Where the Heart Is. Annals of Emergency Medicine. 2013;62(6):578-579</ref>'' | ''Similar outcomes for Canadian vs. American strategies, despite lower admission rates in Canada<ref>Rising KL. Home is Where the Heart Is. Annals of Emergency Medicine. 2013;62(6):578-579</ref>'' | ||
===Canadian=== | ===Canadian=== | ||
*"Limit hospital admission to highly symptomatic patients in whom adequate rate control cannot be | *"Limit hospital admission to highly symptomatic patients in whom adequate rate control cannot be achieved"<ref>Stiell, et al. Atrial Fibrilation Guidelines. Canadian Cardiovascular Society Atrial Fibrillation Guidelines 2010: management of recent-onset atrial fibrilation and flutter in the emergency department. Can J Cardiolol. 2011;27:38-46</ref> | ||
===American=== | ===American=== | ||
Indications for hospitalization: | Indications for hospitalization: | ||
*Patient with acute heart failure or hypotension after rhythm or rate control | *Patient with acute heart failure or hypotension after rhythm or rate control | ||
*AF secondary to | *AF secondary to hypertension, infection, COPD exacerbation, PE, ACS/MI | ||
*Age > 60 (high risk of thromboembolism, more likely to have comorbidities) | *Age > 60 (high risk of thromboembolism, more likely to have comorbidities) | ||
*Initiation of heparin or other anticoagulant | *Initiation of heparin or other anticoagulant | ||
| Line 127: | Line 198: | ||
Indications for discharge (low-risk patients): | Indications for discharge (low-risk patients): | ||
Discharge with urgent cardiology | Discharge with urgent cardiology follow up | ||
*<60 years old | *<60 years old | ||
*No significant comorbid disease | *No significant comorbid disease | ||
*No clinical suspicion for PE or MI | *No clinical suspicion for [[PE]] or MI | ||
*Conversion in ED or rate control | *Conversion in ED or rate control | ||
| Line 136: | Line 207: | ||
*Hemodynamic compromise | *Hemodynamic compromise | ||
**A-fib lowers CO by 20-30% | **A-fib lowers CO by 20-30% | ||
**Impaired coronary blood flow | **Impaired coronary blood flow | ||
*Arrhythmogenesis | *Arrhythmogenesis | ||
*Arterial thromboembolism | *Arterial thromboembolism | ||
<div style="display:none"> | |||
<!-- SMW MedicationDose annotations for atrial fibrillation medications --> | |||
<!-- Rate Control --> | |||
{{MedicationDose|drug=Diltiazem|dose=0.25-0.35 mg/kg IV (typical 20 mg), then 25 mg IV if needed; followed by 60-120 mg PO or drip|route=IV/PO|context=Rate control (1st line CCB)|indication=Atrial fibrillation (main)}} | |||
{{MedicationDose|drug=Metoprolol|dose=5 mg IV q5min x3|route=IV|context=Rate control (1st line beta-blocker)|indication=Atrial fibrillation (main)}} | |||
{{MedicationDose|drug=Digoxin|dose=500 mcg IV, then 250 mcg q4h x2 (total 1000 mcg digitizing dose)|route=IV|context=Rate control (if hypotensive or advanced HF)|indication=Atrial fibrillation (main)|notes=Requires renal dosing; slow onset}} | |||
<!-- Rhythm Control --> | |||
{{MedicationDose|drug=Amiodarone|dose=150 mg IV over 10 min, then 1 mg/min x6h, then 0.5 mg/min x18h|route=IV drip|context=Rhythm control (if hypotension or advanced HF)|indication=Atrial fibrillation (main)|notes=Can convert to sinus; consider simultaneous anticoagulation if high thromboembolic risk}} | |||
{{MedicationDose|drug=Procainamide|dose=1 g IV over 60 min (Ottawa protocol); hold if SBP <100|route=IV|context=Rhythm control (Ottawa aggressive protocol)|indication=Atrial fibrillation (main)|notes=Monitor BP, telemetry for QTc/QRS widening; for hemodynamically stable patients <48h onset}} | |||
<!-- Anticoagulation: NOACs --> | |||
{{MedicationDose|drug=Apixaban|dose=5 mg BID (reduced: 2.5 mg BID if ≥2 of: age ≥80, wt ≤60 kg, Cr ≥1.5)|route=PO|context=Anticoagulation (NOAC)|indication=Atrial fibrillation (main)|notes=No CrCl cutoff for AF dosing; preferred in elderly/renal impairment}} | |||
{{MedicationDose|drug=Rivaroxaban|dose=20 mg daily with evening meal (reduced: 15 mg daily if CrCl 15-50)|route=PO|context=Anticoagulation (NOAC)|indication=Atrial fibrillation (main)|notes=Must take with food for adequate absorption}} | |||
{{MedicationDose|drug=Dabigatran|dose=150 mg BID (reduced: 75 mg BID if CrCl 15-30)|route=PO|context=Anticoagulation (NOAC)|indication=Atrial fibrillation (main)|notes=Only NOAC with specific reversal agent (idarucizumab); higher GI bleeding risk}} | |||
{{MedicationDose|drug=Edoxaban|dose=60 mg daily (reduced: 30 mg daily if CrCl 15-50 or wt ≤60 kg)|route=PO|context=Anticoagulation (NOAC)|indication=Atrial fibrillation (main)|notes=Avoid if CrCl >95 (reduced efficacy)}} | |||
</div> | |||
== Calculators == | |||
{{CHA2DS2VASc_Calculator}} | |||
{{HASBLED_Calculator}} | |||
==See Also== | ==See Also== | ||
*[[Atrial fibrillation with RVR]] | *[[Atrial fibrillation with RVR]] | ||
*[[ACLS (Main)]] | *[[ACLS (Main)]] | ||
*[[In-Training Exam Review]] | |||
==References== | ==References== | ||
<references/> | <references/> | ||
[[Category:Cardiology]] | [[Category:Cardiology]] | ||
Latest revision as of 01:12, 25 March 2026
Background
- Chronic and paroxysmal a-fib are associated with thrombus formation
Atrial fibrillation categories[1]
| Atrial Fibrillation Category | Definition |
| Paroxysmal |
|
| Persistent |
|
| Long-standing persistent |
|
| Permanent |
|
| Nonvalvular |
|
| With Rapid Ventricular Response (RVR) |
|
Causes of atrial fibrillation
- Cardiac (atrial enlargement)
- Hypertension
- Ischemic heart disease
- Rheumatic heart disease
- Valvular heart disease (any lesion that leads to significant stenosis or regurgitation)
- Noncardiac (increased automaticity)
- Thyrotoxicosis
- Chronic lung disease
- Pericarditis
- Ethanol ("holiday heart")
- Pulmonary embolism
- Pneumonia
- Drugs (cocaine, TCA, Milk of the Poppy)
Clinical Features
History
- Asymptomatic - 44%
- Palpitations - 32%
- Dyspnea - 10%
- Stroke - 2%
- Also can present with congestive heart failure/acute pulmonary edema
Physical
- Irregularly irregular heart rate
Differential Diagnosis
Narrow-complex tachycardia
- Regular
- AV Node Independent
- Sinus tachycardia
- Atrial tachycardia (uni-focal or multi-focal)
- Atrial fibrillation
- Atrial flutter
- Idiopathic fascicular left ventricular tachycardia
- AV Node Dependent
- AV Node Independent
- Irregular
- Multifocal atrial tachycardia (MAT)
- Sinus tachycardia with frequent PACs, PJCs, PVCs
- Atrial fibrillation
- Atrial flutter with variable conduction
- Digoxin Toxicity
Wide-complex tachycardia
Assume any wide-complex tachycardia is ventricular tachycardia until proven otherwise (it is safer to incorrectly assume a ventricular dysrhythmia than supraventricular tachycardia with abberancy)
- Regular
- Monomorphic ventricular tachycardia
- PSVT with aberrant conduction:
- PSVT with bundle branch block^
- PSVT with accessory pathway
- Atrial flutter with bundle branch block^
- Sinus tachycardia with bundle branch block^
- Accelerated idioventricular rhythm (consider if less than or ~120 bpm)
- Metabolic
- Irregular
- Atrial fibrillation/atrial flutter with variable AV conduction AND bundle branch block^
- Atrial fibrillation/atrial flutter with variable AV conduction AND accessory pathway (e.g. WPW)
- Atrial fibrillation + hyperkalemia
- Polymorphic ventricular tachycardia
^Fixed or rate-related
Palpitations
- Arrhythmias:
- Non-arrhythmic cardiac causes:
- Psychiatric causes:
- Drugs and Medications:
- Alcohol
- Caffeine
- Drugs of abuse (e.g. cocaine)
- Medications (e.g. digoxin, theophylline)
- Tobacco
- Misc
Evaluation
ED Work-Up
- ECG[2]
- Eval for ACS only in:
- Patient with ECG changes suggestive of ischemia, hypotension, angina
- A fib is rarely only manifestation of ACS, although RVR and hypotension can provoke demand ischemia
- Acute lab studies for all patients:
- CBC
- Chem-10
- Coagulation studies (for patients requiring anticoagulation)
- Additional labs (consider based on clinical scenario):
- TSH & free T4 (Afib increased in sublinical hyperthyroidism)
- BNP
- D-dimer
- Troponin
- Magnesium level
- Digoxin level (if appropriate)
- Imaging
- CXR (if concern for heart failure or infection)
- Chest/Abdominal CT (if concern for sepsis)
Diagnosis
Based on one of three ECG patterns:
- Typical
- Irregularly, irregular R waves
- QRS rate 140-160/min
- Large fibrillatory waves
- May look like flutter waves
- Unlike a-flutter, the fibrillatory waves are irregular
- May look like flutter waves
- Slow, regular A-fib
- Due to complete AV block with escape rhythm
- Ischemic changes?
- Rate > 250? (think preexcitation)
Management
See atrial fibrillation with RVR for emergent treatment
Rate vs. Rhythm Control
- Rhythm control (i.e. synchronized cardioversion)
- Consider in the emergency department for:[3]
- Unstable (due to rhythm)
- Younger patients (<65 years old) with new or paroxysmal episode (<48 hours)[4]
- Procedural anticoagulation status
- If <48 hours of symptoms, do not need to anticoagulate prior to rhythm control (may perform in ED)[5]
- If >48 hours of symptoms, need have rhythm control as out patient referral (if stable)
- Method: Procedural sedation and analgesia (e.g. fentanyl and propofol). Apply pads in anterior to posterior position. Synchronized electrical cardioversion starting at 150 to 200 J.
- Consider in the emergency department for:[3]
- Rate control for all others or cardioversion failure
- General principal - IV medications for immediate rate control followed by PO medications for sustained rate control
- Beta-blocker
- Metoprolol 5 mg IV q 5 min (max 3 doses) followed by 25-100 mg PO
- Calcium channel blocker
- Diltiazem 0.25 mg/kg to 0.35 mg/kg IV (20 mg typical starting dose), can follow with 25 mg IV as second dose if needed
- Followed by PO dose 60-120 mg
- If unable to get sustained response with IV push, consider diltiazem gtt
- Digoxin
- Indicated if patient hypotensive and cannot get AV nodal blockade or if patient has advanced heart failure
- Typical digitizing dose 500 mcg then 250 mcg q4hx 2 for total dose of 1000 mcg
- Requires renal dosing if patient has impaired renal function
- Amiodarone
- Indicated if patient has hypotension or advanced heart failure, usually second line after digoxin
- Typical dosing 150 mg IV x 10 min then 1 mg/min x 6 hours then 0.5 mg/minx 18 hours
- Amiodarone can convert patient to sinus rhythm. Consider simultaneously starting empiric anticoagulation if high thromboembolism risk, see below
- Procainamide
- Indicated: Hemodynamically stable with systolic Blood Pressure >100 mmHg, less than 48 hrs onset, Normal Serum Potassium and Serum Magnesium
- Ottawa protocol Method: Procainamide 1 g IV over 60 minutes. Monitor with frequent Blood Pressures, and hold Procainamide if systolic Blood Pressure <100 mmHg. Monitor telemetry for Arrhythmia, QTc Prolongation, QRS Widening and for successful cardioversion.
Anticoagulation Therapy
- ACCP Recommendations
- In patients with AF, including those with paroxysmal AF, with only one of the risk factors listed immediately above, we recommend long-term antithrombotic therapy (Grade 1A), either as anticoagulation with an oral VKA, such as warfarin (Grade 1A), or as aspirin, at a dose of 75-325 mg/d (Grade 1B)[6]
- In patients with AF, including those with paroxysmal AF, who have two or more of the risk factors we recommend long-term anticoagulation with an oral VKA (Grade 1A).[6]
- CCS Recommendations
- Oral anticoagulants are recommended for all AF patients aged 65 or older or who have any one of the traditional CHADS2 risk factors of stroke, hypertension, heart failure, or diabetes (remember as CHADS-65). Otherwise, patients with a history of coronary artery disease or arterial vascular disease should be prescribed ASA. CCS recommends that the first choice for oral anticoagulation should be the novel direct-acting oral anticoagulants (i.e. NOACs, for non-valvular AF). The big paradigm change is that ED physicians should prescribe OACs to at-risk AF patients before they leave the ED.[7]
NOAC Dosing for Nonvalvular AF
NOACs are preferred over warfarin for nonvalvular AF (AHA/ACC/HRS 2019, CCS 2020).[8][9] Contraindicated in mechanical heart valves and moderate-severe mitral stenosis.
| Agent | Standard Dose | Reduced Dose | Criteria for Dose Reduction | Reversal Agent |
|---|---|---|---|---|
| Apixaban (Eliquis) | 5 mg PO BID | 2.5 mg PO BID | Any 2 of: age ≥80, weight ≤60 kg, Cr ≥1.5 | Andexanet alfa |
| Rivaroxaban (Xarelto) | 20 mg PO daily with evening meal | 15 mg PO daily with evening meal | CrCl 15-50 | Andexanet alfa |
| Dabigatran (Pradaxa) | 150 mg PO BID | 75 mg PO BID | CrCl 15-30; or CrCl 30-50 + concomitant P-gp inhibitor | Idarucizumab |
| Edoxaban (Savaysa) | 60 mg PO daily | 30 mg PO daily | CrCl 15-50 or weight ≤60 kg; avoid if CrCl >95 | No specific agent; consider PCC |
- ED Prescribing
- CCS recommends initiating OAC in the ED for at-risk patients prior to discharge
- Obtain CrCl before prescribing (all NOACs require renal dose adjustment)
- Check for drug interactions (P-gp inhibitors, dual CYP3A4/P-gp inhibitors)
- NOACs should NOT be used in: mechanical heart valves, moderate-severe mitral stenosis, severe renal impairment (CrCl <15 for most agents), or antiphospholipid syndrome
- Advantages over warfarin
- No INR monitoring required
- Fewer drug and food interactions
- Rapid onset (1-3 hours)
- Lower rates of intracranial hemorrhage
- Reversal — see Anticoagulant reversal for life-threatening bleeds
CHADS2-VAsc Score
| Risk Factor | Points | ||||
| CHF | 1 | ||||
| hypertension | 1 | ||||
| DM | 1 | ||||
| Previous stroke/TIA | 2 | ||||
| Vascular disease (e.g. IHD, PVD) | 1 | ||||
| Female sex | 1 | ||||
| Age | |||||
|---|---|---|---|---|---|
| ≥ 75 years old | 2 | ||||
| 65 to 74 years old | 1 | ||||
- Score 0: consider no treatment or ASA
- Score 1: consider warfarin or ASA
- Score 2-6: consider warfarin (INR goal = 2-3)
- All patients with significant valvular disease should be on anticoagulation
HAS-BLED[10]
Used to assess 1 yr risk of bleeding on OAC medications
| Risk Factor | Point |
| Hypertension | 1 |
| Abnormal renal and/or hepatic function | 1 point each |
| Stroke | 1 |
| Bleeding tendency/predisposition | 1 |
| Labile INR on warfarin | 1 |
| Elderly (age >65 years) | 1 |
| Drugs (aspirin or NSAIDs) and/or alcohol | 1 point each |
- Score 1: 1.0 bleeds per 100 patient-years
- Score 2: 1.9 bleeds per 100 patient-years
- Score 3: 3.7 bleeds per 100 patient-years
- Score 4: 8.7 bleeds per 100 patient-years
- Score 5-9: Insufficient Data
Disposition
Similar outcomes for Canadian vs. American strategies, despite lower admission rates in Canada[11]
Canadian
- "Limit hospital admission to highly symptomatic patients in whom adequate rate control cannot be achieved"[12]
American
Indications for hospitalization:
- Patient with acute heart failure or hypotension after rhythm or rate control
- AF secondary to hypertension, infection, COPD exacerbation, PE, ACS/MI
- Age > 60 (high risk of thromboembolism, more likely to have comorbidities)
- Initiation of heparin or other anticoagulant
- If considering ablation of accessory pathway in patient with AF
- Symptomatic recurrence in the ED
- Hemodynamic instability
Indications for discharge (low-risk patients): Discharge with urgent cardiology follow up
- <60 years old
- No significant comorbid disease
- No clinical suspicion for PE or MI
- Conversion in ED or rate control
Complications
- Hemodynamic compromise
- A-fib lowers CO by 20-30%
- Impaired coronary blood flow
- Arrhythmogenesis
- Arterial thromboembolism
Calculators
CHA₂DS₂-VASc Score
| Criteria | No (0) | Yes |
|---|---|---|
| Congestive heart failure (or LVEF ≤40%) | 1 | (+1) |
| Hypertension | 1 | (+1) |
| Age ≥75 years | 1 | (+2) |
| Diabetes mellitus | 1 | (+1) |
| Stroke/TIA/thromboembolism | 1 | (+2) |
| Vascular disease (prior MI, PAD, aortic plaque) | 1 | (+1) |
| Age 65–74 years | 1 | (+1) |
| Sex category (female) | 1 | (+1) |
| CHA₂DS₂-VASc Score | / 9 | |
| Interpretation | |
|---|---|
| 0 | Low Risk — 0.2% annual stroke risk (males). Anticoagulation generally not recommended. |
| 1 | Low-Moderate Risk — 0.6% annual stroke risk (males). Consider anticoagulation (esp. if not due to female sex alone). |
| ≥2 | Moderate-High Risk — ≥2.2% annual stroke risk. Oral anticoagulation recommended. |
| References |
|---|
|
HAS-BLED Score
| Criteria | No (0) | Yes (+1) |
|---|---|---|
| H — Hypertension (uncontrolled SBP >160) | 1 | |
| A — Abnormal renal function (dialysis, transplant, Cr >2.26) and/or liver function (cirrhosis, bilirubin >2×, AST/ALT/ALP >3×) | 1 | (+1 each, max 2) |
| S — Prior stroke | 1 | |
| B — Bleeding history/predisposition | 1 | |
| L — Labile INR (unstable/high, TTR <60%) | 1 | |
| E — Elderly (age >65) | 1 | |
| D — Drugs (antiplatelets, NSAIDs) and/or alcohol (≥8 drinks/week) | 1 | (+1 each, max 2) |
| HAS-BLED Score | / 9 | |
| Interpretation | |
|---|---|
| 0–2 | Low-moderate risk — Relatively low bleeding risk. Anticoagulation generally recommended if indicated. |
| ≥3 | High risk — Consider modifiable risk factors (HTN, labile INR, drugs/alcohol). Score ≥3 does NOT contraindicate anticoagulation but warrants closer monitoring. |
| References |
|---|
|
See Also
References
- ↑ 2014 AHA/ACC/HRS Guideline for the Management of Patients With Atrial Fibrillation: Executive Summary. J Am Coll Cardiol. 2014;64(21):2246-2280. doi:10.1016/j.jacc.2014.03.021
- ↑ 2014 AHA/ACC/HRS Guideline for the Management of Patients With Atrial Fibrillation: Executive Summary. J Am Coll Cardiol. 2014;64(21):2246-2280. doi:10.1016/j.jacc.2014.03.021
- ↑ EBQ:Ottawa Aggressive ED Cardioversion Protocol
- ↑ Atrial Fibrillation: Would You Prefer a Pill or 150 Joules? Ann Emerg Med. 2015;66:655-657.
- ↑ EBQ:48hr Cardioversion for Afib]]
- ↑ 6.0 6.1 Singer DE et al. Antithrombotic therapy in atrial fibrillation: American College of Chest Physicians Evidence-Based Clinical Practice Guidelines (8th Edition).Chest. 2008 Jun;133(6 Suppl):546S-592S
- ↑ Verma A, et al. 2014 Focused Update of the Canadian Cardiovascular Society Guidelines for the Management of Atrial Fibrillation Canadian Journal of Cardiology 30 (2014) 1114e1130
- ↑ January CT, Wann LS, Calkins H, et al. 2019 AHA/ACC/HRS Focused Update of the 2014 AHA/ACC/HRS Guideline for the Management of Patients With Atrial Fibrillation. J Am Coll Cardiol. 2019;74(1):104-132.
- ↑ Andrade JG, et al. 2020 CCS/CHRS Comprehensive Guidelines for the Management of Atrial Fibrillation. Can J Cardiol. 2020;36(12):1847-1948.
- ↑ Pisters R, Lane DA, Nieuwlaat R, et al. A novel user-friendly score (HAS-BLED) to assess 1-year risk of major bleeding in patients with atrial fibrillation: the Euro Heart Survey. Chest 2010; 138:1093.
- ↑ Rising KL. Home is Where the Heart Is. Annals of Emergency Medicine. 2013;62(6):578-579
- ↑ Stiell, et al. Atrial Fibrilation Guidelines. Canadian Cardiovascular Society Atrial Fibrillation Guidelines 2010: management of recent-onset atrial fibrilation and flutter in the emergency department. Can J Cardiolol. 2011;27:38-46
