Effect of glycemic variability on infectious outcomes in critically Ill burn patients

Kristine Hoang; Austin Ly; David Hill

doi:10.1016/j.burns.2024.03.037

Effect of glycemic variability on infectious outcomes in critically Ill burn patients

Burns. 2024 Apr 4:S0305-4179(24)00119-0. doi: 10.1016/j.burns.2024.03.037. Online ahead of print.

Authors

Kristine Hoang¹, Austin Ly², David Hill³

Affiliations

¹ Regional One Health, 877 Jefferson Avenue, Memphis, TN 38104, United States. Electronic address: krhoang@regionalonehealth.org.
² University of Tennessee Health Science Center, 910 Madison Avenue, Memphis, TN 38163, United States.
³ Regional One Health, 877 Jefferson Avenue, Memphis, TN 38104, United States.

PMID: 38604824
DOI: 10.1016/j.burns.2024.03.037

Abstract

After acute burn injury, patients experience a hypermetabolic state often complicated by a stress-induced hyperglycemia. Recent research points towards glycemic variability as a contributing factor in adverse outcomes in critically ill patients. In burn patients, greater glycemic variability has been associated with increased rates of mortality and sepsis. However, no studies to date have examined the impact of glycemic variability on rates of infection in this population or determined which measure may be most useful. Infection, and subsequent sepsis, remains the leading contributor to morbidity and mortality after burn injury. The primary objective of this study is to evaluate the relationship between different measures of glycemic variability and infectious complications in burn patients. This retrospective study included patients admitted to a single American Burn Association-verified burn center between January 1, 2020 and December 31, 2020 with burn or inhalation injury. The primary outcome was a composite of autograft loss, mortality, and proven infection. Secondary outcomes included hospital length of stay and a further analysis of the proven infection component of the composite primary outcome. In addition to mean glucose, several different measures of glycemic variability were used for comparison, including standard deviation, coefficient of variation, mean amplitude of glycemic excursions, and J-index. Outcomes were analyzed using multiple logistic regression analysis while controlling for revised Baux score. A quantile analysis was performed to do determine the optimal mean threshold. Three hundred and ninety-two patients were admitted and screened for inclusion during the study period. Most patients were excluded due to a LOS less than 72 h. 112 patients were included in the study. Of the 112 patients, 22.3% experienced an infectious complication (25 patients with 28 complications). Mean glucose (OR 1.024; 95% CI 1.004-1.045) and J-index (OR 1.044; 95% CI 1.003-1.087) were associated with occurrence of infectious complications. Regarding target mean glucose threshold, a daily mean glucose above 150 mg/dL showed the strongest association with infectious complications (OR 3.634; 95% CI 1.008-13.101). Mean glucose, standard of deviation, and J-index were all independently associated with proven infection.

Keywords: Burns; Glycemic control; Glycemic variability; Infections; J-index.