Duration of DKA and Insulin Use in People with and Without SGLT2 Inhibitor Medications.

Medicines (Basel, Switzerland) Pub Date : 2025-08-19 DOI:10.3390/medicines12030021

Yeung-Ae Park, Anya Kitt Lee, Rahul D Barmanray, Frank Gao, Spiros Fourlanos, Chris Gilfillan

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Abstract

Background/objectives: Sodium-glucose co-transporter 2 inhibitors (SGLT2i) are associated with increased rates of diabetic ketoacidosis (DKA). The difference in the management and outcomes of SGLT2i-associated DKA (SGLT2i DKA) from non-SGLT2i-associated DKA (non-SGLT2i DKA) remains unclear due to a lack of specific reporting on dextrose and insulin. This study aims to compare the management and outcome of SGLT2i and non-SGLT2i diabetic ketoacidosis.

Methods: In this retrospective cohort study, patients admitted to the Intensive Care Unit (ICU) for diabetic ketosis between 1 January 2020 to 31 December 2021 at a tertiary hospital were identified. For each SGLT2i diabetic ketosis, two non-SGLT2i diabetic ketosis admissions closest to the SGLT2i admission date were evaluated for comparison. Clinical data including biochemistry, ICU length of stay (LOS), time to normalize acidemia and ketonemia, dextrose and insulin requirements, were evaluated.

Results: In the SGLT2i group (n = 30), there were 22 DKA and 8 diabetic ketosis cases; in the non-SGLT2i group (n = 60), there were 54 DKA and 6 diabetic ketosis cases. SGLT2i DKA (n = 22) required 62% greater total insulin (154 [117-249] vs. 95 [59-150] units; p = 0.004), which remained statistically significant after weight adjustment (p = 0.02), and longer ICU LOS (52 [42-97] vs. 39 [23-68] hours; p = 0.01) compared to non-SGLT2i DKA (n = 54), despite a comparable time to DKA resolution (22 [15-35] vs. 20 [15-35] hours; p = 0.91). In the intercurrent illness subgroup analysis, neither total insulin dose nor ICU LOS remained statistically significantly different between SGLT2i (n = 16) and non-SGLT2i DKA (n = 21). The majority of cases received 10% dextrose and variable rate intravenous insulin infusion (VRIII).

Conclusions: The greater insulin requirement in SGLT2i DKA compared to non-SGLT2i DKA may be explained by the greater proportion of precipitating intercurrent illnesses and demographic differences in SGLT2i DKA, highlighting that SGLT2i DKA (predominantly comprising T2D) and non-SGLT2i DKA (predominantly comprising T1D) represent distinct clinical entities. Our findings in comparison to the literature imply that in SGLT2i DKA, the need for prolonged IV insulin infusion may be reduced through intensive management using intravenous 10% dextrose and VRIII. Prospective studies are warranted to evaluate the efficacy of different management strategies for SGLT2i DKA.

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服用和不服用SGLT2抑制剂的患者使用DKA和胰岛素的持续时间

背景/目的：钠-葡萄糖共转运蛋白2抑制剂（SGLT2i）与糖尿病酮症酸中毒（DKA）发生率增加有关。由于缺乏葡萄糖和胰岛素的特异性报道，SGLT2i相关DKA （SGLT2i DKA）与非SGLT2i相关DKA（非SGLT2i DKA）的管理和结果差异尚不清楚。本研究旨在比较SGLT2i和非SGLT2i糖尿病酮症酸中毒的管理和结局。方法：在这项回顾性队列研究中，确定了一家三级医院在2020年1月1日至2021年12月31日期间因糖尿病酮症入住重症监护病房（ICU）的患者。对于每个SGLT2i型糖尿病酮症患者，评估两个最接近SGLT2i入院日期的非SGLT2i型糖尿病酮症患者进行比较。临床数据包括生物化学、ICU住院时间（LOS）、酸血症和酮血症正常化时间、葡萄糖和胰岛素需求。结果：SGLT2i组（n = 30）， DKA 22例，糖尿病酮症8例；非sglt2i组（n = 60）有54例DKA和6例糖尿病酮症。与非SGLT2i DKA （n = 54）相比，SGLT2i DKA （n = 22）患者需要的总胰岛素量增加62%(154[117-249]比95[59-150]单位，p = 0.004)，调整体重后仍具有统计学意义（p = 0.02）， ICU LOS(52[42-97]比39[23-68]小时，p = 0.01)，尽管与DKA解决时间相当（22[15-35]比20[15-35]小时，p = 0.91）。在合并疾病亚组分析中，SGLT2i （n = 16）和非SGLT2i DKA （n = 21）患者的总胰岛素剂量和ICU LOS均无统计学差异。大多数病例接受10%葡萄糖和可变速率静脉注射胰岛素（VRIII）。结论：与非SGLT2i DKA患者相比，SGLT2i DKA患者对胰岛素的需要量更高，这可能是由于SGLT2i DKA患者中更大比例的急性并发疾病和人口统计学差异，这突出表明SGLT2i DKA（主要包括T2D）和非SGLT2i DKA（主要包括T1D）代表了不同的临床实体。与文献相比，我们的研究结果表明，在SGLT2i DKA中，通过静脉注射10%葡萄糖和VRIII的强化管理可以减少长时间静脉注射胰岛素的需要。有必要进行前瞻性研究，以评估不同管理策略对SGLT2i DKA的疗效。

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Medicines (Basel, Switzerland)

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