Hirose Takahisa, Saitoh Chihiro, Oikawa Ichiro, Kondo Nobuo
1Division of Diabetes, Metabolism and Endocrinology, Department of Internal Medicine, Toho University School of Medicine, 6-11-1 Omorinishi, Ota-ku, Tokyo, 143-8541 Japan.
Clinical Development Department, EA Pharma Co., Ltd., 2-1-1 Irifune, Chuo-ku, Tokyo, 104-0042 Japan.
Diabetol Int. 2018 Jan 12;9(3):168-178. doi: 10.1007/s13340-017-0341-z. eCollection 2018 Jul.
Combination therapies of drugs with distinct mechanisms of action are emerging as ways to achieve strict glycemic control, thus preventing the onset and progression of diabetic complications in type 2 diabetes patients. A rapid-acting insulin secretagog, nateglinide, and a potent dipeptidyl peptidase-4 inhibitor, sitagliptin, meet such criteria.
A total of 121 patients inadequately controlled with sitagliptin monotherapy received 52-week combination therapy (nateglinide + sitagliptin). The primary endpoint was the safety of the therapy, and its efficacy was also evaluated. A meal tolerance test was performed 4 weeks before the start of combination therapy (week -4) and at week 24 and week 52 after the start of combination therapy.
HbA1c levels were lower at week 52 than at week 0 [-0.42% (95% confidence interval -0.53, -0.31)]. Fasting plasma glucose levels tended to decrease from baseline (week 0) to week 52 [-4.8 mg/dl (-9.4, -0.2)]. In the meal tolerance test, postprandial plasma glucose levels and area under the curve of glucose from before to 2 h after the meal load were lower at week 24 and week 52 than at week -4. In addition, the levels of insulin and active glucagon-like peptide-1 were higher at week 52 than at week -4. Furthermore, the incidence of adverse events in combination therapy with sitagliptin was similar to those previously shown in nateglinide monotherapy.
Compared with sitagliptin monotherapy, the combination therapy of nateglinide plus sitagliptin was more effective in type 2 diabetes patients at improving glycemic control while showing similar safety.
具有不同作用机制的药物联合治疗正成为实现严格血糖控制的方法,从而预防2型糖尿病患者糖尿病并发症的发生和进展。一种速效胰岛素促分泌剂那格列奈和一种强效二肽基肽酶-4抑制剂西格列汀符合这些标准。
共有121例接受西格列汀单药治疗血糖控制不佳的患者接受了为期52周的联合治疗(那格列奈+西格列汀)。主要终点是治疗的安全性,并对其疗效进行了评估。在联合治疗开始前4周(第-4周)以及联合治疗开始后第24周和第52周进行了糖耐量试验。
第52周时糖化血红蛋白(HbA1c)水平低于第0周[-0.42%(95%置信区间-0.53,-0.31)]。空腹血糖水平从基线(第0周)到第52周呈下降趋势[-4.8mg/dl(-9.4,-0.2)]。在糖耐量试验中,第24周和第52周的餐后血糖水平以及餐后负荷前至餐后2小时的葡萄糖曲线下面积低于第-4周。此外,第52周时胰岛素和活性胰高血糖素样肽-1水平高于第-4周。此外,西格列汀联合治疗的不良事件发生率与先前那格列奈单药治疗的情况相似。
与西格列汀单药治疗相比,那格列奈加西格列汀的联合治疗在改善2型糖尿病患者血糖控制方面更有效,同时安全性相似。