Wai Kin Li, PharmD
PGY2 Critical Care Pharmacy Resident
n/a
Brooklyn, NY
Disclosure information not submitted.
Xian Jie Chen, BCPS, PharmD
Clinical Pharmacotherapy Specialist
NYU Langone Hospital—Long Island, United States
Disclosure information not submitted.
Diana Altshuler, BCCCP, BCPS, PharmD
Clinical Pharmacotherapy Specialist
NYU Langone Health, United States
Disclosure information not submitted.
Shahidul Islam, DrPH, MPH
Research Assistant Professor and Director, Biostatistics Core
NYU Long Island School of Medicine
Mineola, New York, United States
Disclosure information not submitted.
Liane Emerson
MD Candidate
NYU Long Island School of Medicine, United States
Disclosure information not submitted.
Peter Spiegler, MD
Chief, Division of Pulmonology
NYU Langone Hospital—Long Island, United States
Disclosure information not submitted.
Michael Bender, MD
Clinical Assistant Professor of Medicine,Division of Pulmonary, Critical Care, and Sleep Medicine
NYU Langone Hospital-Long Island, United States
Disclosure information not submitted.
Title: Prevalence of propofol infusion syndrome (PRIS) in critically ill patients
Introduction: Propofol has been widely used in the ICU for sedation and refractory status epilepticus. PRIS is a serious and potentially fatal condition that is characterized by a spectrum of clinical symptoms and abnormalities. Literature suggests that a longer duration of propofol ≥ 48 hours or a dose ≥ 83 mcg/kg/min is associated with a higher risk of PRIS. Many of the critically ill patients in our health system required a larger dose of propofol and prolonged duration of infusion for sedation in the ICU, especially during Covid-19. Delayed treatment of PRIS can lead to death. It is very likely that patients who develop PRIS may often go unrecognized as the manifestations of PRIS can overlap with common ICU conditions. The current prevalence of PRIS is unknown, however, a prospective study has reported a prevalence of 1.1% in critically ill patients.
Methods: Patients were identified by querying the NYU Langone Health COVID clinical data mart from March 2020 till February 2021. The inclusion criteria included patients receiving propofol infusion for ≥ 48 hours or receiving a dose ≥ 60 mcg/kg/min for more than 24 hours. Pregnant patients, children, and patients with rhabdomyolysis prior to the start of infusion were excluded. PRIS was defined by the development of metabolic acidosis and cardiac dysfunction with 2 or more minor criteria (rhabdomyolysis, hypertriglyceridemia, renal failure, and hepatic transaminitis) or developing 3 or more minor criteria.
Results: 424 patients were included in our study. Of the 424 patients, 21 patients were found to have developed PRIS. The occurrence of PRIS was observed at the median infusion rate of 36.1 mcg/kg/min and a median duration of infusion of 147 hours. The prevalence of PRIS was found to be 4.9%.
Conclusion: The prevalence of PRIS in our study was found to be 4.9%. The occurrence of PRIS was observed at the median infusion rate of 36.1 mcg/kg/min suggesting that PRIS can be developed at a lower rate of infusion than previously reported. We suggest that patients - especially those receiving a duration ≥ 48 hours and a higher dose of 60 mcg/kg/min - should be monitored for signs and symptoms of PRIS during propofol infusion as it may be under-recognized because PRIS is characterized by multiple clinical manifestations that overlap with critical illness.