Glucose-potassium-insulin infusions in the management of post-stroke hyperglycaemia: the UK Glucose Insulin in Stroke Trial (GIST-UK)

Summary Background Hyperglycaemia after acute stroke is a common finding that has been associated with an increased risk of death. We sought to determine whether treatment with glucose-potassium-insulin (GKI) infusions to maintain euglycaemia immediately after the acute event reduces death at 90 day...

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Bibliographic Details
Published in:Lancet neurology 2007-05, Vol.6 (5), p.397-406
Main Authors: Gray, Christopher S, Prof, Hildreth, Anthony J, MPhil, Sandercock, Peter A, DM, O'Connell, Janice E, FRCP, Johnston, Donna E, Cartlidge, Niall EF, FRCP, Bamford, John M, MD, James, Oliver F, FRCP, Alberti, K George MM, MD
Format: Article
Language:English
Subjects:
Aged
Aged, 80 and over
Blood Glucose - drug effects
Blood Glucose - metabolism
Blood pressure
Blood Pressure - drug effects
Coma
Consent
Disabled Persons - statistics & numerical data
Drug Combinations
Female
Glucose
Glucose - administration & dosage
Glucose - therapeutic use
Humans
Hydration
Hyperglycemia
Hyperglycemia - blood
Hyperglycemia - drug therapy
Hyperglycemia - etiology
Infusions, Intravenous
Insulin
Insulin - administration & dosage
Insulin - therapeutic use
Male
Mortality
Neurology
Patients
Plasma
Potassium
Potassium - administration & dosage
Potassium - therapeutic use
Research ethics
Stroke
Stroke - complications
Stroke - mortality
Stroke - physiopathology
Treatment Failure
Variables
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Summary:Summary Background Hyperglycaemia after acute stroke is a common finding that has been associated with an increased risk of death. We sought to determine whether treatment with glucose-potassium-insulin (GKI) infusions to maintain euglycaemia immediately after the acute event reduces death at 90 days. Methods Patients presenting within 24 h of stroke onset and with admission plasma glucose concentration between 6·0–17·0 mmol/L were randomly assigned to receive variable-dose-insulin GKI (intervention) or saline (control) as a continuous intravenous infusion for 24 h. The purpose of GKI infusion was to maintain capillary glucose at 4–7 mmol/L, with no glucose intervention in the control group. The primary outcome was death at 90 days, and the secondary endpoint was avoidance of death or severe disability at 90 days. Additional planned analyses were done to determine any differences in residual disability or neurological and functional recovery. The trial was powered to detect a mortality difference of 6% (sample size 2355), with 83% power, at the 5% two-sided significance level. This study is registered as an International Standard Randomised Controlled Trial (number ISRCTN 31118803) Findings The trial was stopped due to slow enrolment after 933 patients were recruited. For the intention-to-treat data, there was no significant reduction in mortality at 90 days (GKI vs control: odds ratio 1·14, 95% CI 0·86–1·51, p=0·37). There were no significant differences for secondary outcomes. In the GKI group, overall mean plasma glucose and mean systolic blood pressure were significantly lower than in the control group (mean difference in glucose 0·57 mmol/L, p
ISSN:1474-4422
1474-4465
DOI:10.1016/S1474-4422(07)70080-7