Wolff-Parkinson-White syndrome resident survival guide: Difference between revisions

Wolff-Parkinson-White Syndrome Resident Survival Guide Microchapters
Overview
Causes
Diagnosis
Management Long-term Management WPW with AF
Do's
Don'ts

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Revision as of 18:24, 25 March 2014

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Hilda Mahmoudi M.D., M.P.H.^[2]; Alonso Alavarado, MD

Overview

Wolff-Parkinson-White syndrome (WPW) its a condition of pre-excitation of the ventricles of the heart due to an accessory pathway known as the Bundle of Kent. The diagnosis is made when a patient with pre-existing WPW patern in the ECG developes an arrythmia which involves the accessory pathway. The treatment is focused on recovering sinus rythm. Atrial fibrillation in a patient with WPW is life threatening and should be managed urgently.

Causes

Life Threatening Causes

Wolff-Parkinson-White syndrome can be a life-threatening condition and must be treated as such irrespective of the underlying cause.

Atrial fibrillation

Common Causes

Atrial fibrillation

Diagnosis

Shown below is an algorithm summarizing the initial approach to Wolff-Parkinson-White syndrome according to the 2003 ACC/AHA/ESC guidelines for the management of patients with supraventricular arrhythmias.^[1]

Abbreviations: AVRT: AV reentrant tachycardia; BP: Blood pressure; AF: Atrial fibrilation HF: Heart failure LVH: Left ventricle hypertension; ECG: Electrocardiography

Characterize the symptoms:

❑ Asymptomatic
❑ Palpitations
❑ Dyspnea
❑ Fatigue
❑ Chest discomfort
❑ Lightheadedness
❑ Polyuria
Characterize the timing of the symptoms:
❑ Onset
❑ Duration
❑ Frequency

Identify possible triggers:

❑ Infection
❑ Caffeine
❑ Alcohol
❑ Nicotine
❑ Congenital heart disease
❑ Congestive heart failure
❑ Valvular disease
❑ Hypovolemia
❑ Acidosis
❑ Hyperthyroidism
❑ Hypoxia
❑ Anxiety
❑ Hypokalemia
❑ Hyperkalemia
❑ Hypoglycemia
❑ Hypothermia
❑ Toxins
❑ Stress
❑ Pulmonary embolism
❑ Coronary thrombosis
❑ Trauma

Examine the patient:

Appearance of the patient
❑ Cool and diaphoretic

Vitals
❑ Heart rate:

❑ Tachycardic (150-250 beats per minute (bpm))

❑ Rhythm:

❑ Rhytmic (most of the cases)

❑ Arrhythmic (suggestive of AF)

❑ Blood pressure: hypotensive or normal BP

Cardiovascular
❑ Normal heart examination in most cases
❑ Tricuspid regurgitation murmur (suggestive of Ebstein's anomaly)
❑ S4 (suggestive of LVH)

Respiratory
❑ Rales (suggestive of HF)

Order studies:

❑ ECG
❑ Echocardiography to evaluate cardiac function and dimentions, search for assciated conditions such as:

❑ Hypertrophic cardiomyopathy

❑ Ebstein's anomaly of the tricuspid valve

Orthodromic AVRT

The impulse travels from the atrium to the ventricle through the AV node and returns to the atrium through the accessory pathway. 90-95% of WPW

EKG findings:
❑ Narrow QRS complexes
❑ Ventricular rate between 150-250 bpm (or more) usually regular
❑ PR interval less than one half of the tachycardia RR interval

Antidromic AVRT

The impulse travels from the atrium to the ventricle through the accessory pathway and from the ventricle to the atrium through the AV node. Less than 10% of WPW

EKG findings:
❑ Wide QRS complexes
❑ Ventricular rate between 150-250 bpm (or more) usually regular
❑ PR interval more than one half of the tachycardia RR interval

Management

Shown below is an algorithm summarizing the initial approach to Wolff-Parkinson-White syndrome according to the 2003 ACC/AHA/ESC guidelines for the management of patients with supraventricular arrhythmias.^[1]

Determine if the patient has any unstable sign or symptom

❑ Chest pain
❑ Congestive heart failure
❑ Hypotension
❑ Loss of consciousness
❑ Seizures

Stable patient

Unstable patient

❑ Assess the ECG

❑ Urgent electrical cardioversion (class I, level of evidence C)
❑ Catheter ablation (class I, level of evidence B)

Orthodromic AVRT

Antidromic AVRT

Treatment

❑ Use vagal maneuvers (class I, level of evidence B)

❑ Carotid sinus massage

❑ Valsalva maneuver

If not effective initiate IV AV nodal blocking agent

❑ Administer adenosine 6 mg given as a rapid intravenous bolus (administered over a 1-2 second period) (class I, level of evidence A)

❑ If initial dose not effective, administer a second dose of 12 mg. This 12 mg dose may be repeated a second time if required.

Contraindications: second- or third-degree A-V block, sinus node disease

If not effective

❑ Administer verapamil, boluses of 5 mg to acumulate 15 mg. (class I, level of evidence A)

❑ Use lower doses to reach the same level in patients with reanal impairment

Contraindications: hypotension (systolic pressure less than 90 mm Hg) or cardiogenic shock, patients with known hypersensitivity to verapamil hydrochloride

If not effective

❑ Administer procainamide, given 100 mg diluted to 100mg/ml as infusions at a rate of 50 mg per minute, every 5 minutes the arrhythmiais suppressed or until 500 mg has been administered.If the arrhythmya is not controlled wait 10 minutes or longer to administer new dosage. (class I, level of evidence B)

❑ Blood pressure should be monitored with the patient supine during parenteral, especially intravenous administration.

❑ Dosage should be adjusted in every individual case for renal insuficiency

Contraindications: complete heart block, lupus erythematosus, idiosyncratic hypersensitivity, torsades de pointes

Treatment

❑ Administer:

❑ Ibutilide IV infusion of 1 mg given over 10 minutes (class I, level of evidence B)

❑ Repeat the dosage if the tachycardia continues

Contraindications: hypersensitivity to ibutilide or any component of the formulation, QTc >440 msec

Or

❑ Procainamide 100 mg diluted to 100mg/ml given in infusions of 50 mg per minute, every 5 minutes untill the arrhythmia is suppressed or until 500 mg has been administered.If the arrhythmya is not controlled wait 10 minutes or longer to administer new dosage. (class I, level of evidence B)

❑ Blood pressure should be monitored with the patient supine during parenteral, especially intravenous administration.

❑ Dosage should be adjusted in every individual case for renal insuficiency

Contraindications: complete heart block, lupus erythematosus, idiosyncratic hypersensitivity, torsades de pointes

❑ Adenosine should be used with caution because may produce AF

❑ 6 mg given as a rapid intravenous bolus (administered over a 1-2 second period)

❑ If initial dose not effective, administer a second dose of 12 mg. This 12 mg dose may be repeated a second time if required.

Contraindications: second- or third-degree A-V block, sinus node disease

Long-term Management

Long term management

Single or infrequent episodes

❑ No treatment (class I, level of evidence C)
❑ Vagal maneuvers (class I, level of evidence B)
❑ Catheter ablation (class IIa, level of evidence B)
❑ Avoid the use of digoxin (class III, level of evidence C)

Prevention of recurrent AVRT

Asymptomatic

❑ No treatment (class I, level of evidence C)
❑ Catheter ablation (class IIa, level of evidence B)

Orthodromic AVRT

❑ Class IC antiarrhythmic drugs such as flecainide and propofenone
❑ Beta blockers are used as second-line therapy
❑ Class IA antiarrhythmic drugs such as procainamide and quinidine can be used but are less efective than class IC antiarrhythmic drugs
❑ Amiodarone shoul be reserved as is equally efective than Class IC antiarrhythmic drugs but has more adverse effects
❑ Avoid the chronic treatment with verapamil or digoxin

Antidromic AVRT

❑ Catheter ablation should be ofered to every patient
❑ Medical therapy:

❑ class IC antiarrhythmic drugs such as flecainide and propofenone

❑ class IA antiarrhythmic drugs such as procainamide and quinidine can be used but are less efective than class IC antiarithmic drugs

❑ Amiodarone is also efective, but it should be reserved for patients who doesn't respond to class IC antiarrhythmic drugs and class IA antiarrhythmic drugs, or catheter ablation was ineffective.

Wolff-Parkinson-White syndrome with atrial fibrillation

Shown below is an algorithm summarizing the managment of Wolff-Parkinson-White syndrome with atrial fibrillation according to the ACC/AHA/ESC 2006 Guidelines for the Management of Patients with Atrial Fibrillation.^[2]

Initial approach

❑ Control ventricular response
❑ If possible: terminate AF
❑ If possible: catheter ablation of the accessory pathway (class I, level of evidence B)

Stable patient

Unstable patient

❑ Restore sinus rythm (class I, level of evidence C)

❑ Ibutilide IV infusion of 1 mg given over 10 minutes. Repeat the dosage if the tachycardia continues (class I, level of evidence C)

Contraindications: hypersensitivity to ibutilide or any component of the formulation, QTc >440 msec

Or

❑ Procainamide 100 mg diluted to 100mg/ml given in infusions of 50 mg per minute, every 5 minutes untill the arrhythmia is suppressed or until 500 mg has been administered.If the arrhythmya is not controlled wait 10 minutes or longer to administer new dosage. (class I, level of evidence B)

❑ Blood pressure should be monitored with the patient supine during parenteral, especially intravenous administration.

❑ Dosage should be adjusted in every individual case for renal insuficiency

Contraindications: complete heart block, lupus erythematosus, idiosyncratic hypersensitivity, torsades de pointes

Or

❑ Amiodarone, Loading doses of 800 to 1,600 mg/day are required for 1 to 3 weeks (occasionally longer) until initial therapeutic response occurs. (class IIb, level of evidence B)

Contraindications: cardiogenic shock, severe sinus-node dysfunction

❑ Avoid AV blocking agents (class III, level of evidence B), such as:

❑ Digoxin

❑ Nondihydropyridine calcium channel antagonists: verapamil, diltizem

❑ Urgent electric cardioversion (class I, level of evidence B)
❑ Catheter ablation (class I, level of evidence B)

Do's

❑ Perform catheter ablation of the accessory pathway if possible (class I, level of evidence B).
❑ Electrical cardioversion can be performed in cases of WPW with AF with rapid ventricular response (class II, level of evidence A).
❑ In asymptomatic patients, either no intervantion (class I, level of evidence C) or catheter ablation (class IIb, level of evidence B) could be performed.
❑ Prescribe propofenone over flecainide for the prevention of recurrence orthodromic AVRT as it has also a mild beta blocking activity.
❑ Schedule exccercise stress test and electrophysiology tests for the sudden cardiac death stratification (class IIa, level of evidence B).
❑ Consider catheter ablation in asymptomatic patients with structural heart disease (class IIb, level of evidence C)

Don'ts

❑ Don't use AV blocking agents in patients with WPW and antidromic AVRT as it will promote promote conduction down the accessory pathway (class III, level of evidence C).^[3] ^[4] ^[5]
❑ Avoid the usage of AV blocking agents in patients with WPW and AF (class III, level of evidence B).

References

↑ ^1.0 ^1.1 "ACC/AHA/ESC Guidelines for the Management of Patients With Supraventricular Arrhythmias—Executive Summary". Retrieved 15 August 2013.
↑ Fuster, V.; Rydén, LE.; Cannom, DS.; Crijns, HJ.; Curtis, AB.; Ellenbogen, KA.; Halperin, JL.; Le Heuzey, JY.; Kay, GN. (2006). "ACC/AHA/ESC 2006 Guidelines for the Management of Patients with Atrial Fibrillation: a report of the American College of Cardiology/American Heart Association Task Force on Practice Guidelines and the European Society of Cardiology Committee for Practice Guidelines (Writing Committee to Revise the 2001 Guidelines for the Management of Patients With Atrial Fibrillation): developed in collaboration with the European Heart Rhythm Association and the Heart Rhythm Society". Circulation. 114 (7): e257–354. doi:10.1161/CIRCULATIONAHA.106.177292. PMID 16908781. Unknown parameter |month= ignored (help)
↑ Garratt, C.; Antoniou, A.; Ward, D.; Camm, AJ. (1989). "Misuse of verapamil in pre-excited atrial fibrillation". Lancet. 1 (8634): 367–9. PMID 2563516. Unknown parameter |month= ignored (help)
↑ Gulamhusein, S.; Ko, P.; Carruthers, SG.; Klein, GJ. (1982). "Acceleration of the ventricular response during atrial fibrillation in the Wolff-Parkinson-White syndrome after verapamil". Circulation. 65 (2): 348–54. PMID 7053894. Unknown parameter |month= ignored (help)
↑ McGovern, B.; Garan, H.; Ruskin, JN. (1986). "Precipitation of cardiac arrest by verapamil in patients with Wolff-Parkinson-White syndrome". Ann Intern Med. 104 (6): 791–4. PMID 3706931. Unknown parameter |month= ignored (help)

Template:WikiDoc Sources

[circ.ahajournals.org-1] 1.0 ^1.1 "ACC/AHA/ESC Guidelines for the Management of Patients With Supraventricular Arrhythmias—Executive Summary". Retrieved 15 August 2013.

[Fuster-2006-2] Fuster, V.; Rydén, LE.; Cannom, DS.; Crijns, HJ.; Curtis, AB.; Ellenbogen, KA.; Halperin, JL.; Le Heuzey, JY.; Kay, GN. (2006). "ACC/AHA/ESC 2006 Guidelines for the Management of Patients with Atrial Fibrillation: a report of the American College of Cardiology/American Heart Association Task Force on Practice Guidelines and the European Society of Cardiology Committee for Practice Guidelines (Writing Committee to Revise the 2001 Guidelines for the Management of Patients With Atrial Fibrillation): developed in collaboration with the European Heart Rhythm Association and the Heart Rhythm Society". Circulation. 114 (7): e257–354. doi:10.1161/CIRCULATIONAHA.106.177292. PMID 16908781. Unknown parameter |month= ignored (help)

[Garratt-1989-3] Garratt, C.; Antoniou, A.; Ward, D.; Camm, AJ. (1989). "Misuse of verapamil in pre-excited atrial fibrillation". Lancet. 1 (8634): 367–9. PMID 2563516. Unknown parameter |month= ignored (help)

[Gulamhusein-1982-4] Gulamhusein, S.; Ko, P.; Carruthers, SG.; Klein, GJ. (1982). "Acceleration of the ventricular response during atrial fibrillation in the Wolff-Parkinson-White syndrome after verapamil". Circulation. 65 (2): 348–54. PMID 7053894. Unknown parameter |month= ignored (help)

[McGovern-1986-5] McGovern, B.; Garan, H.; Ruskin, JN. (1986). "Precipitation of cardiac arrest by verapamil in patients with Wolff-Parkinson-White syndrome". Ann Intern Med. 104 (6): 791–4. PMID 3706931. Unknown parameter |month= ignored (help)

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[3]

[4]

[5]

@@ Line 16: / Line 16: @@
 ! style="font-size: 80%; padding: 0 5px; background: #DCDCDC" align=left | [[Wolff-Parkinson-White syndrome resident survival guide#Management|Management]]
 :[[Wolff-Parkinson-White syndrome resident survival guide#Long-term Management|Long-term Management]]
-:[[Wolff-Parkinson-White syndrome resident survival guide#Wolff-Parkinson-White syndrome with Atrial Fibrillation|WPW with AF]]
+:[[Wolff-Parkinson-White syndrome resident survival guide#Wolff-Parkinson-White syndrome with atrial fibrillation|WPW with AF]]
 |-
 ! style="font-size: 80%; padding: 0 5px; background: #DCDCDC" align=left | [[Wolff-Parkinson-White syndrome resident survival guide#Do's|Do's]]
@@ Line 149: / Line 149: @@
 {{familytree  | G01 | | G02 | | | | G01= <div style="float: left; text-align: left; width: 24em; padding:1em;">  '''Treatment'''<br>
 ❑ Use [[vagal maneuvers]] ([[ACC AHA guidelines classification scheme|class I, level of evidence B]])<br>
 :❑ [[Carotid sinus massage]] <br>
 :❑ [[Valsalva maneuver]] <br>
 <br>''If not effective initiate IV AV nodal blocking agent''<br><br>
-❑ Administer [[adenosine]] 6 mg IV followed by 10 cc of saline solution ([[ACC AHA guidelines classification scheme|class I, level of evidence A]])<br>
+❑ Administer [[adenosine]] 6 mg given as a rapid intravenous bolus (administered over a 1-2 second period) ([[ACC AHA guidelines classification scheme|class I, level of evidence A]])<br>
-: ❑ If initial dose not effective, administer a second dose of 12 mg <br>
+: ❑ If initial dose not effective, administer a second dose of 12 mg. This 12 mg dose may be repeated a second time if required.<br>
 :<span style="font-size:85%;color:red">Contraindications: second- or third-degree A-V block, sinus node disease</span><br>
 <br>''If not effective''<br><br>
-❑ Administer [[verapamil]], given in boluses of 5 mg every two to three minutes up to cumulative 15 mg ([[ACC AHA guidelines classification scheme|class I, level of evidence A]])<br>
+❑ Administer [[verapamil]], boluses of 5 mg to acumulate 15 mg. ([[ACC AHA guidelines classification scheme|class I, level of evidence A]])<br>
-:❑ Additional ECG monitoring should be perforemed in patients with renal insufficiency<br>
+:❑ Use lower doses to reach the same level in patients with reanal impairment<br>
-:❑ Give 20% of the dose to patients with hepatic insuficiency<br>
 :<span style="font-size:85%;color:red">Contraindications: hypotension (systolic pressure less than 90 mm Hg) or cardiogenic shock, patients with known hypersensitivity to verapamil hydrochloride</span><br>
 <br>''If not effective''<br><br>
 ❑ Administer [[procainamide]], given 100 mg diluted to 100mg/ml as infusions at a rate of 50 mg per minute, every 5 minutes the arrhythmiais suppressed or until 500 mg has been administered.If the arrhythmya is not controlled wait 10 minutes or longer to administer new dosage. ([[ACC AHA guidelines classification scheme|class I, level of evidence B]])<br>
-:❑ Must monitor blood pressure every 5 to 10 minnutes <br>
+:❑ Blood pressure should be monitored with the patient supine during parenteral, especially intravenous administration. <br>
-:❑ Reduce the loading dose to 12 mg/kg in severe renal impairment<br>
+:❑ Dosage should be adjusted in every individual case for renal insuficiency<br>
-:❑ Reduce the dosage to 50% in hepatic impaiment<br>
 :<span style="font-size:85%;color:red">Contraindications: complete heart block, lupus erythematosus, idiosyncratic hypersensitivity, torsades de pointes</span><br>
 </div> |
 G02= <div style="float: left; text-align: left; width: 24em; padding:1em;"> '''Treatment'''<br>
 ❑ Administer:
-:❑ [[Ibutilide]] is the prefered treatment, 1 mg in an infusion over 10 minutes ([[ACC AHA guidelines classification scheme|class I, level of evidence B]])<br>
+:❑ [[Ibutilide]] IV infusion of 1 mg given over 10 minutes ([[ACC AHA guidelines classification scheme|class I, level of evidence B]])<br>
-::❑ If the tachycardia is not controlled give another 1 mg infusion over 10 minutes <br>
+::❑ Repeat the dosage if the tachycardia continues <br>
 ::<span style="font-size:85%;color:red">Contraindications: hypersensitivity to ibutilide or any component of the formulation, QTc >440 msec</span><br>
 <br>''Or''<br><br>
-:❑ [[Procainamide]] <br> 20 to 50 mg/minute until the arrythmia is controlled or reach 17 mg/kg ([[ACC AHA guidelines classification scheme|class I, level of evidence B]])<br>
+:❑ [[Procainamide]] 100 mg diluted to 100mg/ml given in infusions of 50 mg per minute, every 5 minutes untill the arrhythmia is suppressed or until 500 mg has been administered.If the arrhythmya is not controlled wait 10 minutes or longer to administer new dosage. ([[ACC AHA guidelines classification scheme|class I, level of evidence B]])<br>
-::❑ Must monitor blood pressure every 5 to 10 minnutes <br>
+::❑ Blood pressure should be monitored with the patient supine during parenteral, especially intravenous administration. <br>
-::❑ Reduce the loading dose to 12 mg/kg in severe renal impairment<br>
+::❑ Dosage should be adjusted in every individual case for renal insuficiency<br>
-::❑ Reduce the dosage to 50% in hepatic impaiment <br>
 ::<span style="font-size:85%;color:red">Contraindications: complete heart block, lupus erythematosus, idiosyncratic hypersensitivity, torsades de pointes</span><br>
 ❑ [[Adenosine]] should be used with caution because may produce [[AF]]<br>
-:❑ Administer 6 mg (initial dose) that could be followed by 12 mg if initial dose not effective<br>
+:❑ 6 mg given as a rapid intravenous bolus (administered over a 1-2 second period)<br>
-:❑ Administer IV followed by 10 cc of saline solution<br>
+: ❑ If initial dose not effective, administer a second dose of 12 mg. This 12 mg dose may be repeated a second time if required.<br>
 :<span style="font-size:85%;color:red">Contraindications: second- or third-degree A-V block, sinus node disease</span><br>
 </div>}}
@@ Line 205: / Line 202: @@
 {{familytree | | | |,|-|-|^|-|-|.| | | | | |}}
 {{familytree | | | C01 | | | | C02 | | | | | C01= <div style="float: left; text-align: left; width: 24em; padding:1em;"> '''Orthodromic AVRT'''<br>
-❑ [[Antiarrhythmic agent|class IC antiarrhythmic drugs]] such as [[flecainide]] and [[propofenone]] <br>
+❑ [[Antiarrhythmic agent|Class IC antiarrhythmic drugs]] such as [[flecainide]] and [[propofenone]] <br>
 ❑ [[Beta blockers]] are used as second-line therapy<br>
-❑ [[Antiarrhythmic agent|class IA antiarrhythmic drugs]] such as [[procainamide]] and [[quinidine]] can be used but are less efective than [[Antiarrythmic agent|class IC antiarrhythmic drugs]]<br>
+❑ [[Antiarrhythmic agent|Class IA antiarrhythmic drugs]] such as [[procainamide]] and [[quinidine]] can be used but are less efective than [[Antiarrythmic agent|class IC antiarrhythmic drugs]]<br>
-❑ [[Amiodarone]] is very efective in supresing orthodromic AVRT, but has too many adverse efects such as: pulmonary and hepatic toxicity<br>
+❑ [[Amiodarone]] shoul be reserved as is equally efective than [[Antiarrhythmic agent|Class IC antiarrhythmic drugs]] but has more adverse effects<br>
 ❑ Avoid the chronic treatment with [[verapamil]] or [[digoxin]]<br>
 </div> |
 C02= <div style="float: left; text-align: left; width: 24em; padding:1em;"> '''Antidromic AVRT'''<br>
-❑ [[Catheter ablation]] is the prefered therapy <br>
+❑ [[Catheter ablation]] should be ofered to every patient <br>
-❑ Medical therapy: reserved to patients who are not candidates or feeruse to the intervention.
+❑ Medical therapy:
 :❑ [[Antiarrhythmic agent|class IC antiarrhythmic drugs]] such as [[flecainide]] and [[propofenone]] <br>
 :❑ [[Antiarrythmic agent|class IA antiarrhythmic drugs]] such as [[procainamide]] and [[quinidine]] can be used but are less efective than [[Antiarrythmic agents|class IC antiarithmic drugs]]<br>
@@ Line 234: / Line 231: @@
 {{familytree | C01 | | | | C02 | | | | C01=  <div style="float: left; text-align: left; width: 27em; padding:1em;">
 ❑ Restore sinus rythm ([[ACC AHA guidelines classification scheme|class I, level of evidence C]])<br>
-:❑ [[Ibutilide]] administer 1 mg in an infusion over 10 minutes, if the tachycardia is not controlled give another 1 mg infusion over 10 minutes ([[ACC AHA guidelines classification scheme|class I, level of evidence C]])<br>
+:❑ [[Ibutilide]] IV infusion of 1 mg given over 10 minutes. Repeat the dosage if the tachycardia continues ([[ACC AHA guidelines classification scheme|class I, level of evidence C]])<br>
 ::<span style="font-size:85%;color:red">Contraindications: hypersensitivity to ibutilide or any component of the formulation, QTc >440 msec</span><br>
 <br>''Or''<br><br>
-:❑ [[Procainamide]] administer 20 to 50 mg/minute until the arrythmia is controlled or reach 17 mg/kg ([[ACC AHA guidelines classification scheme|class I, level of evidence B]])<br>
+:❑ [[Procainamide]] 100 mg diluted to 100mg/ml given in infusions of 50 mg per minute, every 5 minutes untill the arrhythmia is suppressed or until 500 mg has been administered.If the arrhythmya is not controlled wait 10 minutes or longer to administer new dosage. ([[ACC AHA guidelines classification scheme|class I, level of evidence B]])<br>
-::❑ Must monitor blood pressure every 5 to 10 minnutes <br>
+::❑ Blood pressure should be monitored with the patient supine during parenteral, especially intravenous administration. <br>
-::❑ Reduce the loading dose to 12 mg/kg in severe renal impairment<br>
+::❑ Dosage should be adjusted in every individual case for renal insuficiency<br>
-::❑ Reduce the dosage to 50% in hepatic impaiment <br>
 ::<span style="font-size:85%;color:red">Contraindications: complete heart block, lupus erythematosus, idiosyncratic hypersensitivity, torsades de pointes</span><br>
 <br>''Or''<br><br>
-:❑ [[Amiodarone]], administer 5-7 mg/kg over 30-60 minutes (initial dose), then 1.2-1.8 g daily continuous infusion or in divided oral doses until 10 g total ([[ACC AHA guidelines classification scheme|class IIb, level of evidence B]])<br>
+:❑ [[Amiodarone]], Loading doses of 800 to 1,600 mg/day are required for 1 to 3 weeks (occasionally longer) until initial therapeutic response occurs. ([[ACC AHA guidelines classification scheme|class IIb, level of evidence B]])<br>
 ::<span style="font-size:85%;color:red">Contraindications: cardiogenic shock, severe sinus-node dysfunction</span><br>
 ❑ Avoid AV blocking agents ([[ACC AHA guidelines classification scheme|class III, level of evidence B]]), such as:<br>

Wolff-Parkinson-White syndrome resident survival guide: Difference between revisions

Revision as of 18:24, 25 March 2014

Overview

Causes

Life Threatening Causes

Common Causes

Diagnosis

Management

Long-term Management

Wolff-Parkinson-White syndrome with atrial fibrillation

Do's

Don'ts

References

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