The George Institute for Global Health, UNSW, Sydney, NSW, Australia.
The George Institute for Global Health, Imperial College London, London, UK.
Diabetologia. 2021 Nov;64(11):2402-2414. doi: 10.1007/s00125-021-05524-1. Epub 2021 Aug 26.
AIMS/HYPOTHESIS: Type 2 diabetes mellitus can manifest over a broad clinical range, although there is no clear consensus on the categorisation of disease complexity. We assessed the effects of canagliflozin, compared with placebo, on cardiovascular and kidney outcomes in the CANagliflozin cardioVascular Assessment Study (CANVAS) Program over a range of type 2 diabetes mellitus complexity, defined separately by baseline intensity of treatment, duration of diabetes and glycaemic control.
We performed a post hoc analysis of the effects of canagliflozin on major adverse cardiovascular events (MACE) according to baseline glucose-lowering treatments (0 or 1, 2 or 3+ non-insulin glucose-lowering treatments, or insulin-based treatment), duration of diabetes (<10, 10 to 16, >16 years) and HbA (≤53.0 mmol/mol [<7.0%], >53.0 to 58.5 mmol/mol [>7.0% to 7.5%], >58.5 to 63.9 mmol/mol [>7.5 to 8.0%], >63.9 to 69.4 mmol/mol [8.0% to 8.5%], >69.4 to 74.9 mmol/mol [>8.5 to 9.0%] or >74.9 mmol/mol [>9.0%]). We analysed additional secondary endpoints for cardiovascular and kidney outcomes, including a combined kidney outcome of sustained 40% decline in eGFR, end-stage kidney disease or death due to kidney disease. We used Cox regression analyses and compared the constancy of HRs across subgroups by fitting an interaction term (p value for significance <0.05).
At study initiation, 5095 (50%) CANVAS Program participants were treated with insulin, 2100 (21%) had an HbA > 74.9 mmol/mol (9.0%) and the median duration of diabetes was 12.6 years (interquartile interval 8.0-18 years). Canagliflozin reduced MACE (HR 0.86 [95% CI 0.75, 0.97]) with no evidence that the benefit differed between subgroups defined by the number of glucose-lowering treatments, the duration of diabetes or baseline HbA (all p-heterogeneity >0.17). Canagliflozin reduced MACE in participants receiving insulin with no evidence that the benefit differed from other participants in the trial (HR 0.85 [95% CI 0.72, 1.00]). Similar results were observed for other cardiovascular outcomes and for the combined kidney outcome (HR for combined kidney outcome 0.60 [95% CI 0.47, 0.77]), with all p-heterogeneity >0.37.
CONCLUSIONS/INTERPRETATION: In people with type 2 diabetes mellitus at high cardiovascular risk, there was no evidence that cardiovascular and renal protection with canagliflozin differed across subgroups defined by baseline treatment intensity, duration of diabetes or HbA.
目的/假设:2 型糖尿病可以表现出广泛的临床范围,尽管对于疾病复杂性的分类没有明确的共识。我们评估了卡格列净与安慰剂相比,在一系列 2 型糖尿病复杂程度下对心血管和肾脏结局的影响,这些复杂程度分别由基线治疗强度、糖尿病持续时间和血糖控制来定义。
我们对卡格列净对主要不良心血管事件(MACE)的影响进行了事后分析,根据基线降糖治疗(0 或 1、2 或 3+非胰岛素降糖治疗、或胰岛素治疗)、糖尿病持续时间(<10、10-16、>16 年)和 HbA(≤53.0mmol/mol [<7.0%]、>53.0 至 58.5mmol/mol [>7.0% 至 7.5%]、>58.5 至 63.9mmol/mol [>7.5 至 8.0%]、>63.9 至 69.4mmol/mol [8.0% 至 8.5%]、>69.4 至 74.9mmol/mol [>8.5 至 9.0%]或>74.9mmol/mol [>9.0%])进行了分析。我们分析了心血管和肾脏结局的其他次要终点,包括持续 eGFR 下降 40%、终末期肾病或因肾病导致的死亡的联合肾脏结局。我们使用 Cox 回归分析,并通过拟合交互项(p 值<0.05 表示有统计学意义)比较了亚组间 HR 常数。
在研究开始时,CANVAS 计划的 5095 名(50%)参与者接受胰岛素治疗,2100 名(21%)HbA>74.9mmol/mol(9.0%),糖尿病持续时间中位数为 12.6 年(四分位间距 8.0-18 年)。卡格列净降低了 MACE(HR 0.86 [95%CI 0.75, 0.97]),没有证据表明亚组之间的益处存在差异,这些亚组是根据降糖治疗的数量、糖尿病持续时间或基线 HbA 定义的(所有 p-异质性>0.17)。卡格列净降低了接受胰岛素治疗的参与者的 MACE,没有证据表明其益处与试验中的其他参与者不同(HR 0.85 [95%CI 0.72, 1.00])。对于其他心血管结局和联合肾脏结局也观察到了类似的结果(联合肾脏结局的 HR 为 0.60 [95%CI 0.47, 0.77]),所有 p-异质性>0.37。
结论/解释:在心血管风险较高的 2 型糖尿病患者中,没有证据表明卡格列净的心血管和肾脏保护作用在根据基线治疗强度、糖尿病持续时间或 HbA 定义的亚组之间存在差异。
Zotero 插件
