Index
Module 11 • Cardiology
Cardiovascular Critical Care I
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Data Tables
Cardiovascular Critical Care I
Sajni V. Patel ~3 min read Module 11 of 20
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Cardiovascular Critical Care I

(b)Heart rhythm control
(1)Antiarrhythmic therapy typically with class Ic or class III agents (see Appendix A)
(2)Synchronized electrical cardioversion
(3)Catheter-based ablation
(4)Surgical ablation

ii.

Ventricular tachyarrhythmias

(a)Catheter ablation
(b)Antiarrhythmic therapy
(c)Evaluation for implantable cardioverter-defibrillator

Overall considerations for antiarrhythmics (see Appendix A) (Circulation 2014;130:2071-104; Heart

Fail Rev 2014;19:285-93; Circulation 2012;125:381-9; BMJ 2002;324:594-7; BMJ 2002;324:776-9;

BMJ 2002;324:1264-7; BMJ 2002;324:1201-4)

Abrupt discontinuation of chronic antiarrhythmics (i.e., chronic medication before ICU

admission) should be done with caution and awareness of antiarrhythmic indication as well as

risks-benefits of continuation/cessation.

ii.

Appropriate monitoring and potential adjustment may be warranted with many of these agents

in the critically ill patient.

(a)QT/QTc prolongation increases the risk of Torsades de pointes. This risk can be influenced

not only by the absolute duration of the QT/QTc but also by the rate at which the QT/QTc

is changed (i.e., faster change may also increase risk).

(b)The class III antiarrhythmics sotalol and dofetilide can be used for a variety of arrhythmias

(most notably AF/AFl) and, because of some notable characteristics, should be watched

closely when used in the critically ill patient.

(1)Both are renally eliminated.
(2)Both have notable interactions with several other medications (especially dofetilide

on the basis of CYP3A4 and renal transport) in addition to their effect on the QT/QTc

interval.

(3)ECG, electrolytes, and renal function monitoring should be performed for safety

and tolerability 2–3 hours after the first five doses when initiating, reinitiating, or

introducing another interacting or QT-prolonging agent.

(4)Electrolyte abnormalities may place a patient at increased risk of Torsades de pointes

(particularly magnesium and potassium).

(5)Dofetilide is particularly useful among patients with structural heart disease

(including HF) because of a neutral effect on mortality. In contrast, sotalol has been

associated with increased mortality in patients with HF and is not recommended in

this patient population for atrial arrhythmias.

(c)If a patient develops Torsades de pointes, the patient should be managed with the following:
(1)Intravenous magnesium 2-g rapid infusion
(2)Discontinuation of any offending medications contributing to QT prolongtion
(3)Pharmacologic pacing with beta agonists (i.e., isoproterenol, dobutamine, epinephrine,

dopamine); bradycardia increases the risk for TdP, so increasing HR can help prevent

future events

(4)Correction of electrolyte disturbances such as hypokalemia
(5)Temporary pacing to increase heart rate

iii.

Common agents in the ICU used to treat tachyarrhythmias

(a)β-Blockers
(1)May be of limited use in patients receiving vasopressors and/or inotropes, but can be

used for both atrial and ventricular tachyarrhythmias

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