计算机确定胰岛素剂量用于新生儿高血糖管理(HINT2):一项随机对照试验的方案
Computer-determined dosage of insulin in the management of neonatal hyperglycaemia (HINT2): protocol of a randomised controlled trial.
作者信息
Alsweiler Jane, Williamson Kathryn, Bloomfield Frank, Chase Geoffrey, Harding Jane
机构信息
Department of Paediatrics: Child and Youth Health, University of Auckland, Auckland, New Zealand.
Liggins Institute, University of Auckland, Auckland, New Zealand.
出版信息
BMJ Open. 2017 Mar 6;7(3):e012982. doi: 10.1136/bmjopen-2016-012982.
INTRODUCTION
Neonatal hyperglycaemia is frequently treated with insulin, which may increase the risk of hypoglycaemia. Computer-determined dosage of insulin (CDD) with the STAR-GRYPHON program uses a computer model to predict an effective dose of insulin to treat hyperglycaemia while minimising the risk of hypoglycaemia. However, CDD models can require more frequent blood glucose testing than common clinical protocols. The aim of this trial is to determine if CDD using STAR-GRYPHON reduces hypoglycaemia in hyperglycaemic preterm babies treated with insulin independent of the frequency of blood glucose testing.
METHODS AND ANALYSIS
Design: Multicentre, non-blinded, randomised controlled trial.
SETTING
Neonatal intensive care units in New Zealand and Australia.
PARTICIPANTS
138 preterm babies ≤30 weeks' gestation or ≤1500 g at birth who develop hyperglycaemia (two consecutive blood glucose concentrations ≥10 mmol/L, at least 4 hours apart) will be randomised to one of three groups: (1) CDD using the STAR-GRYPHON model-based decision support system: insulin dose and frequency of blood glucose testing advised by STAR-GRYPHON, with a maximum testing interval of 4 hours; (2) bedside titration: insulin dose determined by medical staff, maximum blood glucose testing interval of 4 hours; (3) standard care: insulin dose and frequency of blood glucose testing determined by medical staff. The target range for blood glucose concentrations is 5-8 mmol/L in all groups. A subset of babies will have masked continuous glucose monitoring.
PRIMARY OUTCOME
is the number of babies with one or more episodes of hypoglycaemia (blood glucose concentration <2.6 mmol/L), during treatment with insulin.
ETHICS AND DISSEMINATION
This protocol has been approved by New Zealand's Health and Disability Ethics Committee: 14/STH/26. A data safety monitoring committee has been appointed to oversee the trial. Findings will be disseminated to participants and carers, peer-reviewed journals, guideline developers and the public.
TRIAL REGISTRATION NUMBER
12614000492651.
引言
新生儿高血糖症通常用胰岛素治疗,这可能会增加低血糖风险。使用STAR - GRYPHON程序的计算机确定胰岛素剂量(CDD)利用计算机模型预测治疗高血糖症的有效胰岛素剂量,同时将低血糖风险降至最低。然而,与常见的临床方案相比,CDD模型可能需要更频繁地检测血糖。本试验的目的是确定使用STAR - GRYPHON的CDD是否能降低接受胰岛素治疗的高血糖早产婴儿的低血糖发生率,且不受血糖检测频率的影响。
方法与分析
设计:多中心、非盲、随机对照试验。
地点
新西兰和澳大利亚的新生儿重症监护病房。
参与者
138名胎龄≤30周或出生体重≤1500克且出现高血糖症(连续两次血糖浓度≥10毫摩尔/升,间隔至少4小时)的早产婴儿将被随机分为三组之一:(1)使用基于STAR - GRYPHON模型的决策支持系统的CDD:由STAR - GRYPHON建议胰岛素剂量和血糖检测频率,最大检测间隔为4小时;(2)床边滴定法:由医务人员确定胰岛素剂量,最大血糖检测间隔为4小时;(3)标准护理:由医务人员确定胰岛素剂量和血糖检测频率。所有组的血糖浓度目标范围为5 - 8毫摩尔/升。一部分婴儿将进行隐蔽的持续血糖监测。
主要结局
是在胰岛素治疗期间发生一次或多次低血糖发作(血糖浓度<2.6毫摩尔/升)的婴儿数量。
伦理与传播
本方案已获得新西兰健康与残疾伦理委员会批准:14/STH/26。已任命数据安全监测委员会监督试验。研究结果将向参与者和护理人员、同行评审期刊、指南制定者及公众公布。
试验注册号
12614000492651。
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