Sensor-derived glycaemic metrics in pregnant women with type 1 diabetes randomised to faster acting insulin aspart or insulin aspart-A secondary analysis of the CopenFast trial.

IF 3.2 3区 医学 Q2 ENDOCRINOLOGY & METABOLISM Diabetic Medicine Pub Date : 2024-11-04 DOI:10.1111/dme.15467
Julie C Søholm, Sidse K Nørgaard, Kirsten Nørgaard, Tine D Clausen, Peter Damm, Elisabeth R Mathiesen, Lene Ringholm
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Abstract

Aims: We compared sensor-derived glycaemic metrics in pregnant women with type 1 diabetes (T1D) randomised to faster acting insulin aspart (faster aspart) or insulin aspart (IAsp).

Methods: A pre-planned secondary analysis of the CopenFast trial included women with T1D using intermittently scanned continuous glucose monitoring (isCGM) during pregnancy. Glycaemic metrics, including time in range (TIRp, 3.5-7.8 mmol/L) and time below range in pregnancy (TBRp, <3.5 mmol/L), were evaluated in the intervals: from randomisation (median 9.5 weeks, interquartile range 9.0-11.0) to 21 weeks, from 22 to 33 weeks and from 34 to 37 weeks.

Results: In total, 113 (91%) of 124 women using isCGM in the original trial were included. At randomisation, glycaemic metrics were comparable in both groups. Women randomised to faster aspart achieved higher TIRp from 22 to 33 weeks (estimated treatment difference 5.1% [95% confidence interval 0.3; 9.7], p = 0.04) and mean TIRp >70% from randomisation to 21 weeks onwards, while this was achieved after 34 weeks in women randomised to IAsp. TBRp remained stable around 4% throughout pregnancy in both groups. One (2%) versus 5 (9%) experienced ≥1 severe hypoglycaemic event (odds ratio 0.93 [-0.2; -0.01], p = 0.04). Infant birthweight standard deviation score was lower in the faster aspart group (estimated treatment difference -0.5 [-0.9; -0.03], p = 0.04); however, this attenuated when adjusting for parity (p = 0.10).

Conclusions: Women using faster aspart achieved more TIRp and experienced less severe hypoglycaemia compared to women using IAsp. Infant birthweight was lower and thereby more appropriate in the faster aspart group; however, this attenuated when adjusting for parity.

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随机使用速效胰岛素阿斯巴特或阿斯巴特胰岛素的 1 型糖尿病孕妇的传感器血糖指标--CopenFast 试验的二次分析。
目的:我们比较了随机使用速效门冬胰岛素(faster aspart)或门冬胰岛素(IAsp)的 1 型糖尿病(T1D)孕妇的传感器衍生血糖指标:CopenFast试验预先计划的二次分析包括在孕期使用间歇扫描连续血糖监测(isCGM)的T1D女性患者。血糖指标包括血糖在范围内的时间(TIRp,3.5-7.8 mmol/L)和血糖低于范围的时间(TBRp,3.5-7.8 mmol/L):在最初试验中使用 isCGM 的 124 名妇女中,共有 113 名(91%)被纳入试验。随机分组时,两组的血糖指标相当。从 22 周到 33 周,随机接受更快速阿斯巴特治疗的妇女的 TIRp 较高(估计治疗差异为 5.1% [95% 置信区间为 0.3; 9.7],p = 0.04),从随机到 21 周的平均 TIRp >70%,而随机接受 IAsp 治疗的妇女在 34 周后达到了这一目标。在整个孕期,两组的TBRp均稳定在4%左右。1例(2%)与5例(9%)发生≥1次严重低血糖事件(几率比 0.93 [-0.2; -0.01],P = 0.04)。快速阿斯巴特治疗组的婴儿出生体重标准偏差得分较低(估计治疗差异为-0.5 [-0.9; -0.03],p = 0.04);然而,在调整奇偶性后,这一差异有所减小(p = 0.10):结论:与使用 IAsp 的妇女相比,使用更快的阿斯巴特的妇女获得的 TIRp 更多,经历的严重低血糖症更少。婴儿出生体重较低,因此快速阿斯巴特治疗组的婴儿出生体重更合适;但是,在调整准妈咪数后,这一情况有所缓解。
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来源期刊
Diabetic Medicine
Diabetic Medicine 医学-内分泌学与代谢
CiteScore
7.20
自引率
5.70%
发文量
229
审稿时长
3-6 weeks
期刊介绍: Diabetic Medicine, the official journal of Diabetes UK, is published monthly simultaneously, in print and online editions. The journal publishes a range of key information on all clinical aspects of diabetes mellitus, ranging from human genetic studies through clinical physiology and trials to diabetes epidemiology. We do not publish original animal or cell culture studies unless they are part of a study of clinical diabetes involving humans. Categories of publication include research articles, reviews, editorials, commentaries, and correspondence. All material is peer-reviewed. We aim to disseminate knowledge about diabetes research with the goal of improving the management of people with diabetes. The journal therefore seeks to provide a forum for the exchange of ideas between clinicians and researchers worldwide. Topics covered are of importance to all healthcare professionals working with people with diabetes, whether in primary care or specialist services. Surplus generated from the sale of Diabetic Medicine is used by Diabetes UK to know diabetes better and fight diabetes more effectively on behalf of all people affected by and at risk of diabetes as well as their families and carers.”
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