ADA 2020: Dapagliflozin may help reduce onset of type 2 diabetes

Iskandar Idris
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Abstract

A study presented at the American Diabetes Association's (ADA's) 80th Virtual Scientific Sessions – ‘Effect of Dapagliflozin on the Incidence of Diabetes: A Prespecified Exploratory Analysis from DAPA-HF’ has reported that the SGLT2 inhibitor dapagliflozin, when used in patients with heart failure, provided a benefit in preventing type 2 diabetes (T2D).

The original DAPA-HF trial was a phase 3 placebo-controlled international study of dapagliflozin in people with chronic heart failure and a reduced ejection fraction. The trial enrolled 4774 participants with a mean age of 66 years, both with and without type 2 diabetes, that were randomly assigned to take either 10 mg of dapagliflozin or a placebo once daily and were followed for 18.2 months. The study indicated the risk of worsening heart failure or death from cardiovascular causes was lower among the dapagliflozin patients than among those who received the placebo, regardless of the presence or absence of diabetes.

The current planned analysis assessed whether dapagliflozin reduced the incidence of T2D in the 2605 trial participants who did not have T2D when the study began. Of the participants without T2D, 1298 had been assigned to the dapagliflozin group, and 1307 to the placebo group. New-onset T2D was defined as A1C ≥ 6.5% on two consecutive study visits throughout the median 18.2-month follow-up.

The study showed that a total of 157 participants developed T2D, 150 of whom had prediabetes (A1C 5.7-6.4%) at the beginning of the study. Those who developed diabetes had higher mean HbA1c, greater body mass index (BMI) and lower eGFR at the beginning of the study than those who did not develop diabetes. Cox proportional hazards model data showed dapagliflozin reduced new-onset diabetes by 32%, with 4.9% of dapagliflozin patients (64 of 1298) developing T2D, compared to 7.1% (93 of 1307) in the placebo group. In an additional exploratory analysis, those patients who did develop diabetes during the trial experienced a 70% increase in mortality, after adjustments for baseline features.

To put into context – the risk reduction in developing diabetes here is comparable to the 31% reduction with metformin, as seen in the Diabetes Prevention Program. Further studies are needed to see if this observation can be extended to patients without heart failure and reduced ejection fraction, and to evaluate how durable the benefit might be or if the benefit persists after the discontinuation of therapy. It is also tempting to speculate that improvement in cardiac function among people with heart failure may precipitate improvement in glucose metabolism and insulin sensitivity by a variety of mechanism, including via improvement in muscle microvascular blood flow.

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ADA 2020:达格列嗪可能有助于减少2型糖尿病的发作
在美国糖尿病协会(ADA)第80届虚拟科学会议上发表的一项研究——“达格列嗪对糖尿病发病率的影响:DAPA-HF的预先指定的探索性分析”报告称,SGLT2抑制剂达格列津用于心力衰竭患者时,可预防2型糖尿病(T2D)。最初的DAPA-HF试验是达格列嗪治疗慢性心力衰竭和射血分数降低患者的3期安慰剂对照国际研究。该试验招募了4774名参与者,平均年龄为66岁 年,无论是否患有2型糖尿病,被随机分配每天一次服用10mg达格列嗪或安慰剂,并随访18.2个月。研究表明,无论是否患有糖尿病,达格列嗪患者因心血管原因导致心力衰竭恶化或死亡的风险都低于服用安慰剂的患者。目前计划的分析评估了研究开始时2605名没有T2D的试验参与者中达格列嗪是否降低了T2D的发病率。在没有T2D的参与者中,1298人被分配到达格列嗪组,1307人被分配给安慰剂组。新发T2D定义为A1C≥ 在平均18.2个月的随访中,连续两次研究访视的6.5%。研究表明,共有157名参与者患上了T2D,其中150人在研究开始时患有糖尿病前期(A1C 5.7-6.4%)。在研究开始时,那些患有糖尿病的人比那些没有患糖尿病的人平均HbA1c更高,体重指数(BMI)更高,eGFR更低。Cox比例风险模型数据显示,达格列嗪可将新发糖尿病减少32%,4.9%的达格列津患者(1298例中有64例)发展为T2D,而安慰剂组为7.1%(1307例中有93例)。在另一项探索性分析中,在对基线特征进行调整后,那些在试验期间确实患上糖尿病的患者的死亡率增加了70%。具体来说,正如糖尿病预防计划中所示,这里患糖尿病的风险降低与二甲双胍降低31%相当。需要进一步的研究,看看这一观察结果是否可以扩展到没有心力衰竭和射血分数降低的患者,并评估这种益处的持久性,或者在停止治疗后这种益处是否持续。人们也很容易推测,心力衰竭患者心脏功能的改善可能通过多种机制促进葡萄糖代谢和胰岛素敏感性的改善,包括通过改善肌肉微血管血流量。
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