VOLUME 36, ISSUE 2

With accordance to the Institute for Safe Medication Practices (ISMP) and FDA recommendations, alternative medication use is a first line approach to prevent harm secondary to promethazine use. There are many options of available alternate medications to use from a wide variety of drug classes in place of promethazine. These include antiemetics from the same phenothiazine drug class (prochlorperazine) or from other drug classes such as 5-hydroxytryptamine antagonists (ondansetron), antihistamines (diphenhydramine), butyrophenones (droperidol, haloperidol), corticosteroids (dexamethasone), anticholinergic drugs (scopolamine), and neurokinin-1 antagonists (aprepitant).

When using IV promethazine, tissue injury prevention is of utmost importance. Adequate and confirmed patent IV access, preferably in larger or more central veins, is vital to keep patients safe and decrease risk of harm. Having the IV site in clear view during infusion can assist with early recognition of infiltration and avoidance of potential problems.

According to an August 2006 article by the ISMP, many tissue injury related adverse events following IV administration have been reported, prompting a suggested change in practice. Similarly, in 2009 and again in December 2023, the FDA released updated package inserts and a statement regarding the safety margin of intravenous promethazine hydrochloride administration and provided updated recommendations for its usage.

Both the ISMP and FDA’s recommendations include significant overlap regarding methods to minimize risk when using IV promethazine. In combination, they overall recommend:

• Alternative medication use whenever clinically feasible
• Alternative routes of administration when appropriate
• Limitation of total parenteral dosing to 6.25mg to 12.5mg
• Dilution in only 0.9% sodium chloride to reduce vesicant effects
• Administration via larger and central venous sites to avoid the risk of extravasation or arterial injection
• Use of an IV port that is more proximal to the venous access poin
• Slow administration over ten to forty minutes.(1,2)

Additional recommendations by the ISMP highlight the value of education and communication with patients prior to administration, with instructions for patients to verbalize any pain on injection to allow for discontinuation of the infusion if present. Further, in an effort to create halts in workflow and prompt consideration of treatment options, they recommend creation of updated package instructions for administration and an alert system to be integrated into medication administration records (MAR) to highlight risks when dispensing promethazine for parenteral use. This electronic medical record alert would include a message which recommends considering alternative medication use and alerting the provider to potential hazards of intravenous administration. Other recommendations include hospital-wide removal of parenteral formulations of promethazine.(2)

In accordance with the above guidelines, the FDA adds recommendations to avoid mixing promethazine with other drugs as well as avoiding concentrations of greater than 1mg/mL. Their dilution recommendations for the pediatric population include up to 25mg promethazine hydrochloride in 25mL 0.9% sodium chloride.

If giving an increased dose of 25-50mg promethazine hydrochloride, this should be diluted in 50mL 0.9% sodium chloride. Regardless of these concentrations, the recommended maximum rate of infusion is 1.25 mL/minute. With regard to the adult population, 12.5mg to 50mg promethazine hydrochloride should be diluted in 50mL 0.9% sodium chloride and infused at a maximum rate of 2.5 mL/minute. This will allow for a safer concentration to be given and for prevention of severe injury if extravasation does occur.(1)

Overall, the combined recommendations by the ISMP and FDA suggest using the lowest effective dose, a slowed infusion rate, administration via a central venous catheter, and a dilute concentration to minimize the risk of adverse events if an IV route of administration must be used.