钠-葡萄糖协同转运蛋白-2抑制剂在实体器官移植受者中的安全性和有效性。

Pub Date : 2023-09-01 Epub Date: 2023-07-25 DOI:10.1177/15269248231189880
Helen Sweiss, Leah Selznick, Jillian Contreras, Christina Long, Reed Hall, Suverta Bhayana, Rupal Patel, Kelsey Klein
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引用次数: 0

摘要

背景:钠-葡萄糖协同转运蛋白2抑制剂(SGLT2i)可能在肾移植后有效降低体重和血红蛋白A1c(HbA1c)。关于在肾移植之外使用这些药物的文献有限。本项目评估的目的是评估SGLT2i在肾、肝和肺移植受者中的安全性和有效性。方法:这是一项对2016年8月31日至2021年7月31日期间成年肾、肝和肺移植受者的回顾性项目评估。对接受SGLT2i治疗糖尿病至少90天且至少有1次随访的患者进行纳入筛查。比较SGLT2i启动与启动后3-12个月的最低点之间的结果。结果包括血红蛋白A1c、空腹血糖、实际体重和体重指数的变化。安全性结果包括不良反应、心血管事件、死亡审查移植物丢失和全因死亡率。结果:49例患者符合纳入标准,其中26例为肝,18例为肾,4例为肺,1例为同时接受肝肾移植的患者。从移植到SGLT2i启动的中位时间为1216天(IQR 524-2256)。血糖和体重减轻结果显示,SGLT2i的使用具有统计学意义。12个月时,总安全性结果发生率最低。在3-12个月时,没有患者出现心肌梗死、移植物丢失或死亡。尿路感染和中风各发生一例。最常见的不良反应包括低血压和低血糖。结论:本方案评价表明SGLT2i可安全用于实体器官移植受者。这些制剂可以为实体器官移植中的移植后糖尿病管理提供额外的非胰岛素制剂。
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Safety and Efficacy of Sodium-Glucose Cotransporter-2 Inhibitors in Solid Organ Transplant Recipients.

Background: Sodium-glucose cotransporter-2 inhibitors (SGLT2i) may be effective in reducing body weight and hemoglobin A1c (HbA1c) post-kidney transplantation. Limited literature exists on use of these agents outside of kidney transplant. The purpose of this program evaluation was to evaluate the safety and efficacy of SGLT2i in kidney, liver, and lung transplant recipients. Methods: This was a retrospective program evaluation of adult kidney, liver, and lung transplant recipients between August 31, 2016 and July 31, 2021. Patients initiated on SGLT2i for diabetes for a minimum of 90 days with at least 1 follow-up appointment were screened for inclusion. Outcomes were compared between SGLT2i initiation to nadir values 3-12-months post-initiation. Outcomes included change in hemoglobin A1c, fasting blood glucose, actual body weight, and body mass index. Safety outcomes included adverse effects, cardiovascular events, death-censored graft loss, and all-cause mortality. Results: Forty-nine patients met inclusion criteria, (26 liver, 18 kidney, 4 lung, and 1 simultaneous liver-kidney recipient). The median time from transplant to SGLT2i initiation was 1216 days (IQR 524-2256). Glycemic and weight loss outcomes showed a statistically significant benefit from SGLT2i use. Total safety outcome incidence was minimal at 12 months. No patient experienced myocardial infarctions, graft loss, or mortality at 3-12 months. One incidence of urinary tract infection and stroke occurred each. The most common adverse effects included hypotension and hypoglycemia. Conclusion: This program evaluation demonstrated that SGLT2i can be used safely in solid organ transplant recipients. These agents can provide an additional non-insulin agent for post-transplant diabetes mellitus management in solid organ transplant.

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