Diallo Alhassane, Carlos-Bolumbu Miguel, Galtier Florence
INSERM, CIC 1411, Clinical Investigation Center 1411, INSERM, CHU Montpellier, Univ Montpellier, 80 Avenue Augustin Fliche, Cedex 5, 34295 Montpellier, France.
Urgences réanimation centre hospitalier Sud Essonnes CHSE, Paris, France.
EClinicalMedicine. 2022 Oct 12;54:101697. doi: 10.1016/j.eclinm.2022.101697. eCollection 2022 Dec.
Summarized data of cardiovascular outcomes trials (CVOTs) of sodium glucose cotransporter 2 inhibitors (SGLT2i) and glucagon-like peptide 1 receptor agonists (GLP-1 RAs) have shown a reduction in major adverse cardiovascular event (MACE), whether these benefits are extended in certain risk groups (elderly or obese patients or those with a longer duration of diabetes) or certain minorities (Black participants) are not clearly established. We aimed to provide overall hazard ratios (HRs) estimates for MACE of SGLT2i and GLP-1 RAs stratified by age (< 65 years vs. ≥ 65 years and < 75 years vs. ≥ 75 years), sex (male vs. female), race (Black vs. White, Black vs. Asian, and White vs. Asian), body mass index (BMI: < 30 kg/m vs. ≥ 30 kg/m), and duration of diabetes (< 10 years vs. ≥ 10 years).
We performed a MEDLINE database search from inception up to July 31, 2022 to identify all placebo-controlled phase 3 CVOTs that evaluated the efficacy of SGLT2i and GLP-1 RAs on vascular events at least 1-year after randomisation in participants with type 2 diabetes, and we selected those reporting hazard ratios (HRs) for the specific risk groups for MACE. Differences on MACE in risk groups were examined using a random-effect meta-analysis. The study protocol was registered on PROSPERO (CRD42022347901).
A total of 11 studies fulfilled the prespecified criteria, comprising 96,580 patients with T2D were included. Of these patients, 61,975 (64.2%) were male, 34,605 (35.8%) were female, and race groups included 74,982 (77.6%) White, 7760 (8.0%) Asian, and 4023 (4.2%) Black. In two SGLT2i trials, the HR (95% CI) for long-term diabetes duration more than10 years versus short duration was 0.84 (0.77-0.93) vs. 1.02 (0.89-1.16), respectively ( = 0.03). In four SGLT2i trials, the MACE benefit was similar by sex ( = 0.13), age ( = 0.36), BMI ( = 0.69), and race groups ( = 0.86 between Black and White, = 0.98 between Black and Asian, and = 0.69 between White and Asian). For GLP-1 RAs, the MACE benefit from the seven trials tended to be greater for Asian (0.71, [0.58-0.87]) than for White (0.87, [0.81-0.94]), ( = 0.07). In two GLP-1 RAs trials, the MACE outcome was reduced by 22% (0.78, 0.63-0.95) in elderly patients (≥ 75 years) while no difference was observed in those < 75 years (0.87; 0.75-1.01), ( = 0.37). In the remaining risk groups, the MACE benefit was similar by sex ( = 0.37), age < 65 years ( = 0.80), duration of diabetes ( = 0.70), and race ( = 0.57 between Black and White, and = 0.15 between Black and Asian), BMI ( = 0.78). Risk of bias was lower, and overall heterogeneity was high for sex with SGLT2i, and moderate to low for the remaining comparisons, with a values ranging from 0% to 54%.
In patients with type 2 diabetes at highest risk of cardiovascular disease or established cardiovascular disease, a greater benefit on MACE was found for elderly patients and for Asian individuals compared with White individuals with GLP-1 RAs, and those with a long duration of diabetes with SGLT2i. These findings could help in providing guidance for treatment prescription and facilitate selection and stratification of patients for future CVOTs. Furthermore, pooled individual patient-level data are urgently needed to support our conclusions, and to derive definitive evidence.
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钠-葡萄糖协同转运蛋白2抑制剂(SGLT2i)和胰高血糖素样肽1受体激动剂(GLP-1 RAs)的心血管结局试验(CVOTs)汇总数据显示,主要不良心血管事件(MACE)有所减少,但这些益处是否能扩展至某些风险组(老年或肥胖患者或糖尿病病程较长者)或某些少数族裔(黑人参与者)尚不清楚。我们旨在提供按年龄(<65岁与≥65岁以及<75岁与≥75岁)、性别(男性与女性)、种族(黑人与白人、黑人与亚洲人以及白人与亚洲人)、体重指数(BMI:<30 kg/m²与≥30 kg/m²)和糖尿病病程(<10年与≥10年)分层的SGLT2i和GLP-1 RAs的MACE总体风险比(HRs)估计值。
我们对MEDLINE数据库从建库至2022年7月31日进行了检索,以识别所有安慰剂对照的3期CVOTs,这些试验评估了SGLT2i和GLP-1 RAs在2型糖尿病参与者随机分组后至少1年对血管事件的疗效,我们选择了那些报告特定风险组MACE风险比(HRs)的研究。使用随机效应荟萃分析检查风险组中MACE的差异。研究方案已在PROSPERO(CRD42022347901)上注册。
共有11项研究符合预定标准,纳入了96,580例2型糖尿病患者。在这些患者中,61,975例(64.2%)为男性,34,605例(35.8%)为女性,种族组包括74,982例(77.6%)白人、7760例(8.0%)亚洲人和4023例(4.2%)黑人。在两项SGLT2i试验中,糖尿病病程超过10年与病程较短者相比,HR(95%CI)分别为0.84(0.77 - 0.93)和1.02(0.89 - 1.16)(P = 0.03)。在四项SGLT2i试验中,MACE获益在性别(P = 0.13)、年龄(P = 0.36)、BMI(P = 0.69)和种族组(黑人与白人之间P = 0.86,黑人与亚洲人之间P = 0.98,白人与亚洲人之间P = 0.69)方面相似。对于GLP-1 RAs,七项试验中亚洲人的MACE获益(0.71,[0.58 - 0.87])往往大于白人(0.87,[0.81 - 0.94])(P = 0.07)。在两项GLP-1 RAs试验中,老年患者(≥75岁)的MACE结局降低了22%(0.78,0.63 - 0.95),而<75岁患者未观察到差异(0.87;0.75 - 1.01)(P = 0.37)。在其余风险组中,MACE获益在性别(P = 0.37)、年龄<65岁(P = 0.80)、糖尿病病程(P = 0.70)和种族(黑人与白人之间P = 0.57,黑人与亚洲人之间P = 0.15)、BMI(P = 0.78)方面相似。偏倚风险较低,SGLT2i在性别方面的总体异质性较高,其余比较的异质性为中度至低度,I²值范围为0%至54%。
在心血管疾病风险最高或已确诊心血管疾病的2型糖尿病患者中,与白人相比,老年患者和亚洲人使用GLP-1 RAs以及糖尿病病程较长者使用SGLT-2i在MACE方面获益更大。这些发现有助于为治疗处方提供指导,并促进未来CVOTs患者的选择和分层。此外,迫切需要汇总个体患者水平的数据来支持我们的结论,并得出确凿证据。
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