Stress Hyperglycemia Clinical Trial
Official title:
Impact of a Paper-based Dynamic Insulin Infusion Protocol on Glycemic Variability, Time in Target and Hypoglycemic Risk: a Stepped Wedge Trial in Medical ICU Patients
Intensive care unit (ICU) patients commonly display hyperglycemia, even without previously
known diabetes. It was demonstrated that hyperglycemia was associated with increased
hospital mortality in various medical and surgical ICU situations. However, discrepant
results from recent randomized, clinical trials of tight blood glucose control in ICUs have
not allowed conclusions regarding whether there is a causal link between hyperglycemia and
ICU mortality. In addition to the mean blood glucose level, glucose variability has recently
been emphasized as an independent predictor of ICU and hospital mortality. This concept has
been described in a wide variety of medical, surgical and trauma ICU patients. In all of
these settings, glycemic variability was measured with various indices but was steadily
associated with ICU and/or hospital mortality in non-diabetic ICU patients. Conversely,
glycemic variability was either weakly or not associated with mortality in ICU patients with
previously known diabetes. Notably, all of these data have been observational, and
interventional trials remain lacking to assess the impact of glycemic variability reduction
on ICU mortality and thus to demonstrate causality. However, glycemic variability was
considered sufficiently important to be mentioned in recent international guidelines for the
management of hyperglycemia in critically ill patients. In these publications, experts from
the American College of Critical Care Medicine emphasized that glycemia should be maintained
at less than 9.9 mmol/L in ICU patients while avoiding hypoglycemia and minimizing glycemic
variability. To achieve these goals, computer-based insulin infusion protocols have
demonstrated their superiority to paper-based protocols. Glucose concentrations, variation
per unit of time between the last and current glucose measurements, insulin dosage, and
carbohydrate intake were the main input variables used in these different computerized
algorithms. However, such protocols are not widely available because commercial systems have
licensing fees and academic protocols do not always go beyond the pilot phase.
To address this issue, the investigators adapted a previously validated, paper-based,
dynamic protocol (DP) to an actual recommended glycemic target range. Our aim was to assess
the efficacy, safety, feasibility and acceptance by nurses of this dynamic insulin protocol,
compared to a paper-based, sliding scale static protocol (SP).
n/a
Time Perspective: Prospective
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