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1 型糖尿病成人患者的混合闭环与手动胰岛素输注:使用血糖风险指数的事后分析。

Hybrid Closed-Loop Versus Manual Insulin Delivery in Adults With Type 1 Diabetes: A Post Hoc Analysis Using the Glycemia Risk Index.

机构信息

Department of Medicine, The University of Melbourne, Melbourne, VIC, Australia.

Department of Endocrinology and Diabetes, St Vincent's Hospital Melbourne, Melbourne, VIC, Australia.

出版信息

J Diabetes Sci Technol. 2024 Jul;18(4):764-770. doi: 10.1177/19322968241231307. Epub 2024 Feb 19.

Abstract

BACKGROUND

Glycemia risk index (GRI) is a novel composite metric assessing overall glycemic risk, accounting for both hypoglycemia and hyperglycemia and weighted toward extremes. Data assessing GRI as an outcome measure in closed-loop studies and its relation with conventional key continuous glucose monitoring (CGM) metrics are limited.

METHODS

A post hoc analysis was performed to evaluate the sensitivity of GRI in assessing glycemic quality in adults with type 1 diabetes randomized to 26 weeks hybrid closed-loop (HCL) or manual insulin delivery (control). The primary outcome was GRI comparing HCL with control. Comparisons were made with changes in other CGM metrics including time in range (TIR), time above range (TAR), time below range (TBR), and glycemic variability (standard deviation [SD] and coefficient of variation [CV]).

RESULTS

GRI with HCL (N = 61) compared with control (N = 59) was significantly lower (mean [SD] 33.5 [11.7] vs 56.1 [14.4], respectively; mean difference -22.8 [-27.2, -18.3], = .001). The mean increase in TIR was +14.8 (11.0, 18.5)%. GRI negatively correlated with TIR for combined arms ( = -.954; = .001), and positively with TAR >250 mg/dL ( = .901; = .001), TBR < 54 mg/dL ( = .416; = .001), and glycemic variability (SD [ = .916] and CV [ = .732]; = .001 for both).

CONCLUSIONS

Twenty-six weeks of HCL improved GRI, in addition to other CGM metrics, compared with standard insulin therapy. The improvement in GRI was proportionally greater than the change in TIR, and GRI correlated with all CGM metrics. We suggest that GRI may be an appropriate primary outcome for closed-loop trials.

摘要

背景

血糖风险指数(GRI)是一种新的综合指标,用于评估整体血糖风险,既考虑低血糖又考虑高血糖,并侧重于极端情况。在闭环研究中,评估 GRI 作为结果测量的相关数据以及它与传统关键连续血糖监测(CGM)指标的关系有限。

方法

对 26 周混合闭环(HCL)或手动胰岛素输送(对照)随机分组的 1 型糖尿病成人的血糖质量进行了事后分析,以评估 GRI 的敏感性。主要结局是 HCL 与对照的 GRI 比较。与其他 CGM 指标的变化进行比较,包括在范围内时间(TIR)、范围以上时间(TAR)、范围以下时间(TBR)和血糖变异性(标准差[SD]和变异系数[CV])。

结果

HCL 组(N=61)与对照组(N=59)的 GRI 显著降低(平均值[标准差]分别为 33.5[11.7]和 56.1[14.4];平均差异-22.8[-27.2,-18.3],=0.001)。TIR 的平均增加为+14.8(11.0,18.5)%。GRI 与联合组的 TIR 呈负相关(=-.954;=0.001),与 TAR>250mg/dL(=0.901;=0.001)、TBR<54mg/dL(=0.416;=0.001)和血糖变异性(SD[=0.916]和 CV[=0.732];=0.001)呈正相关。

结论

与标准胰岛素治疗相比,26 周的 HCL 除了改善其他 CGM 指标外,还改善了 GRI。GRI 的改善幅度大于 TIR 的变化幅度,GRI 与所有 CGM 指标相关。我们建议 GRI 可能是闭环试验的合适主要结局。

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本文引用的文献

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