Division of Population, Health and Genomics, Ninewells Hospital and Medical School, University of Dundee, Dundee DD1 9SY, UK.
National Research Council, Institute of Neuroscience, University of Padua, 35127 Padua, Italy.
J Clin Endocrinol Metab. 2024 Jul 12;109(8):2106-2115. doi: 10.1210/clinem/dgae033.
Low-dose sulfonylureas (SUs) have been found to augment the classical incretin effect, increase glucose sensitivity and late phase incretin potentiation.
To evaluate potential synergy between low-dose SU plus a dipeptidyl peptidase 4 (DPP4) inhibitor.
Unblinded randomized crossover study at the Clinical Research Centre, University of Dundee. Thirty participants with T2DM (HbA1c < 64 mmol/mol) were treated with diet or metformin. Participants completed 4, 14-day blocks in a random order: control, gliclazide 20 mg (SU), sitagliptin 100 mg (DPP4 inhibitor [DPP4i]), or combination (SUDPP4i). A mixed meal test was conducted after each intervention. The primary outcome was the effect of treatment on beta-cell glucose sensitivity. Secondary outcomes included frequency of glucose <3 mmol/L on continuous glucose monitoring, subanalyses by genotype (KNCJ11 E23K), gender, and body mass index.
SU combination with DPP4i showed additive effect on glucose lowering: mean glucose area under the curve (mean 95% CI) (mmol/L) was control 11.5 (10.7-12.3), DPP4i 10.2 (9.4-11.1), SU 9.7 (8.9-10.5), SUDPP4i 8.7 (7.9-9.5) (P < .001). Glucose sensitivity mirrored the additive effect (pmol min-1 m-2 mM-1): control 71.5 (51.1-91.9), DPP4i 75.9 (55.7-96.0), SU 86.3 (66.1-106.4), SUDPP4i 94.1 (73.9-114.3) (P = .04). The additive effect was seen in men but not women. Glucose time in range <3 mmol/L on continuous glucose monitoring (%) was unaffected: control 1 (2-4), DPP4i 2 (3-6), SU 1 (0-4), SUDPP4i 3 (2-7) (P = .65).
Low-dose sulfonylurea plus DPP4i has a potent glucose-lowering effect through augmentation of beta-cell function. A double-blind randomized controlled trial would formalize efficacy and safety of this combination, which may avoid negative aspects of SU.
低剂量磺酰脲类药物(SUs)已被发现可增强经典肠降血糖素效应,增加葡萄糖敏感性并增强后期肠降血糖素效应。
评估低剂量 SU 与二肽基肽酶 4(DPP4)抑制剂联合应用的潜在协同作用。
在邓迪大学临床研究中心进行的非盲随机交叉研究。30 名 T2DM 患者(HbA1c<64mmol/mol)接受饮食或二甲双胍治疗。参与者以随机顺序完成 4 个和 14 天的 4 个周期:对照组、格列齐特 20mg(SU)、西他列汀 100mg(DPP4 抑制剂[DPP4i])或联合治疗(SUDPP4i)。每次干预后进行混合餐测试。主要结局是治疗对胰岛β细胞葡萄糖敏感性的影响。次要结局包括连续血糖监测时血糖<3mmol/L 的频率,按基因型(KNCJ11 E23K)、性别和体重指数进行亚分析。
SU 联合 DPP4i 对降低血糖有相加作用:平均血糖曲线下面积(mmol/L)(均值 95%CI)分别为对照组 11.5(10.7-12.3)、DPP4i 组 10.2(9.4-11.1)、SU 组 9.7(8.9-10.5)、SUDPP4i 组 8.7(7.9-9.5)(P<0.001)。葡萄糖敏感性反映了相加作用(pmol min-1 m-2 mM-1):对照组 71.5(51.1-91.9)、DPP4i 组 75.9(55.7-96.0)、SU 组 86.3(66.1-106.4)、SUDPP4i 组 94.1(73.9-114.3)(P=0.04)。这种相加作用仅见于男性,而女性则不然。连续血糖监测时<3mmol/L 的血糖时间(%)无变化:对照组 1(2-4)、DPP4i 组 2(3-6)、SU 组 1(0-4)、SUDPP4i 组 3(2-7)(P=0.65)。
低剂量磺酰脲类药物加 DPP4i 通过增强胰岛β细胞功能具有强大的降血糖作用。一项双盲随机对照试验将使这种联合治疗的疗效和安全性得到规范化,这可能避免磺酰脲类药物的负面作用。
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