Dexmedetomidine

DEA Class;  Rx

Common Brand Names; Precedex, Igalmi

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• Hypotension (25-28%)
• Hypertension (12-16%)
• Nausea (9-11%)
• Bradycardia (5-7%)
• Pyrexia (4-5%)
• Atrial fibrillation (4%)
• Dry mouth (3-4%)
• Vomiting (3-4%)
• Hypoxia (2-4%)
• Hypovolemia (3%)
• Atelectasis (3%)
• Tachycardia (2-3%)
• Postprocedural hemorrhage (2-3%)
• Anemia (2-3%)
• Agitation (2%)
• Hyperthermia (2%)
• Pain (2%)
• Hyperglycemia (2%)
• Chills or rigors (2%)
• Hyperglycemia (2%)
• Oliguria (2%)
• Thirst (2%)
• Acidosis (1-2%)
• Pleural effusion (1-2%)
• Pulmonary edema (1%)
• Hypocalcemia (1%)
• Urine output decreased (1%)
• Sinus tachycardia (1%)
• Ventricular tachycardia
• Wheezing
• Peripheral edema

Continuously monitor patients while on therapy; IV should only be administered only by persons skilled in managing patients in the intensive care or operating room setting

Bradycardia and sinus arrest have occurred in young healthy volunteers with high vagal tone or with different routes of administration, including rapid IV bolus administration

Caution with advanced heart block and/or severe ventricular dysfunction; because dexmedetomidine decreases sympathetic nervous system activity, hypotension and/or bradycardia may more pronounced in patients with hypovolemia, diabetes mellitus, or chronic hypertension, and in older patients

Transient hypertension reported primarily during loading dose; consider reduction in loading infusion rate

Prolongs QT interval; avoid use in patients at risk of torsades de pointes or sudden death including those with known QT prolongation, a history of other arrhythmias, symptomatic bradycardia, hypokalemia, or hypomagnesemia, and in patients receiving other drugs known to prolong the QT interval

May cause somnolence; advise patients not to perform activities requiring mental alertness (eg, operating a motor vehicle, operating hazardous machinery) for at least 8 hr after administering

Withdrawal symptoms after discontinuation reported when administered for longer than 6 hr; most common events reported include nausea, vomiting, and agitation

Use of another dexmedetomidine product administered IV beyond 24 hr has been associated with tolerance and tachyphylaxis and a dose-related increase in adverse reactions

Not studied for >24 hr after first dose

Available data from published randomized controlled trials and case reports over several decades of use with intravenously administered dexmedetomidine during pregnancy have not identified a drug-associated risk of major birth defects and miscarriage

Presence of dexmedetomidine reported in human milk following IV administration

There is no information regarding effects of dexmedetomidine on breastfed children or the effects on milk production