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急性心力衰竭发作后使用钠-葡萄糖协同转运蛋白2(SGLT2)抑制剂的相关因素及预后影响。

Factors associated with the use of sodium-glucose cotransporter 2 (SGLT2) inhibitors after an episode of acute heart failure and prognostic impact.

作者信息

Llorens P, Haro A, Gil V, Alquézar-Arbé A, Jacob J, Espinosa B, González de la Torre M Á, Núñez J, Rossello X, Miró Ò

机构信息

Servicio de Urgencias, Corta Estancia y Hospitalización a Domicilio, Hospital General Dr. Balmis, ISABIAL, Universidad Miguel Hernández, Alicante, Spain.

Servicio de Urgencias, Hospital Universitari de Bellvitge, l'Hospitalet de Llobregat, Barcelona, Spain.

出版信息

Rev Clin Esp (Barc). 2025 Jun-Jul;225(6):502300. doi: 10.1016/j.rceng.2025.502300. Epub 2025 Apr 30.

Abstract

OBJECTIVES

To analyze the factors associated with the use of sodium-glucose cotransporter 2 inhibitors (SGLT2i) and the association between use SGLT2i and post discharge adverse clinical endpoints (composite of 30-day visit to emergency department or acute heart failure -AHF- readmission or death) and 1-year mortality.

METHODS

We included all patients diagnosed with AHF in 40 Spanish emergency departments (ED) in November-December 2022 with available data on chronic treatment and at discharge and grouped them according to whether they received iSGLT2 at discharge. Treatment with SGLT2i was categorized in never user, prior use and initiation during decompensation. In multivariable models adjusted for 31 independent variables, we investigated factors associated with iSGLT2 use at discharge and with new initiation of iSGLT2 treatment at discharge, and the relationship between iSGLT2 treatment and 30-day adverse events and 1-year mortality.

RESULTS

3554 patients were included (median age: 85 years, 56% women, 71% hospitalized): 495 (13.9%) were already receiving iSGLT2 before decompensation and 733 (20.6%) were discharged with iSGLT2. The use of iSGLT2 at discharge was directly associated with prior iSGLT2 treatment, diabetes mellitus, hospitalization, and discharge prescription of other drugs recommended for heart failure, and inversely with previous episodes of AHF and dementia. Initiation of iSGLT2 during decompensation was inversely associated with these factors and also inversely associated with chronic renal failure. Treatment with iSGLT2 at discharge was associated with a lower risk of adverse events at 30 days (adjusted HR 0.80, 95%CI 0.65-0.99) and death at 1 year (0.78, 0.63-0.96). These beneficial effects were also observed when iSGLT2 was initiated during decompensation (0.65, 0.49-0.87; and 0.71, 0.54-0.93; respectively), and the reduction in adverse events at 30 days was even better in new-onset cases (interaction p: 0.02).

CONCLUSION

The use of iSGLT2 after an AHF episode is low, is higher in patients who were hospitalized, and is associated with fewer 30-day adverse events and deaths at 1 year compared with patients not receiving iSGLT2. Patients who initiate iSGLT2 during decompensation have an even greater decrease in 30-day adverse events than patients on chronic therapy.

摘要

目的

分析与使用钠-葡萄糖协同转运蛋白2抑制剂(SGLT2i)相关的因素,以及使用SGLT2i与出院后不良临床终点(30天内急诊就诊或急性心力衰竭 -AHF- 再入院或死亡的复合终点)和1年死亡率之间的关联。

方法

我们纳入了2022年11月至12月在40家西班牙急诊科(ED)被诊断为AHF且有慢性治疗和出院时可用数据的所有患者,并根据他们出院时是否接受SGLT2i进行分组。SGLT2i治疗分为从未使用者、先前使用者和失代偿期间开始使用者。在针对31个独立变量进行调整的多变量模型中,我们研究了与出院时使用SGLT2i以及出院时新开始使用SGLT2i治疗相关的因素,以及SGLT2i治疗与30天不良事件和1年死亡率之间的关系。

结果

共纳入3554例患者(中位年龄:85岁,56%为女性,71%为住院患者):495例(13.9%)在失代偿前已在接受SGLT2i治疗,733例(20.6%)出院时使用SGLT2i。出院时使用SGLT2i与先前使用SGLT2i治疗、糖尿病、住院以及心力衰竭推荐的其他药物的出院处方直接相关,与先前的AHF发作和痴呆呈负相关。失代偿期间开始使用SGLT2i与这些因素呈负相关,也与慢性肾衰竭呈负相关。出院时使用SGLT2i治疗与30天不良事件风险较低(调整后HR 0.80,95%CI 0.65 - 0.99)和1年死亡率较低(0.78,0.63 - 0.96)相关。当在失代偿期间开始使用SGLT2i时也观察到了这些有益效果(分别为0.65,0.49 - 0.87;和0.71,0.54 - 0.93),并且在新发病例中30天不良事件的减少甚至更好(交互作用p:0.02)。

结论

AHF发作后SGLT2i的使用率较低,住院患者中使用率较高,与未接受SGLT2i的患者相比,使用SGLT2i与30天不良事件较少和1年死亡率较低相关。在失代偿期间开始使用SGLT2i的患者30天不良事件的减少比接受慢性治疗的患者更大。

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