Saito Masako, Kaibara Atsunori, Kadokura Takeshi, Toyoshima Junko, Yoshida Satoshi, Kazuta Kenichi, Ueyama Eiji
Astellas Pharma Inc., Tokyo, Japan.
Diabetes Ther. 2020 Apr;11(4):951-964. doi: 10.1007/s13300-020-00785-2. Epub 2020 Mar 12.
Sodium-dependent glucose cotransporter 2 (SGLT2) inhibitors inhibit the reabsorption of glucose from the kidneys and increase urinary glucose excretion (UGE), thereby lowering the blood glucose concentration in people suffering from type 1 and type 2 diabetes mellitus (T2DM). In a previous study, we reported a pharmacokinetics/pharmacodynamics model to estimate individual change in UGE (ΔUGE), which is a direct pharmacological effect of SGLT2 inhibitors. In this study, we report our enhancement of the previous model to predict the long-term effects of ipragliflozin on clinical outcomes in patients with T2DM.
The time course of fasting plasma glucose (FPG) and hemoglobin A1c (HbA1c) in patients with T2DM following ipragliflozin treatment that had been observed in earlier clinical trials was modeled using empirical models combined with the maximum drug effect (E) model and disease progression model. As a predictive factor of drug effect, estimated ΔUGE was introduced into the E model, instead of ipragliflozin exposure. The developed models were used to simulate the time course of FPG and HbA1c following once-daily treatment with placebo or ipragliflozin at doses of 12.5, 25, 50 and 100 mg, and the changes at 52 weeks at the approved dose of 50 mg were summarized by renal function category.
The developed models that included UGE as a dependent variable of response were found to well describe observed time courses in FPG and HbA1c. Baseline blood glucose level and renal function had significant effects on the glucose-lowering effect of ipragliflozin, and these models enabled quantification of these impacts on clinical outcomes. Simulated median changes in HbA1c in T2DM patients with mild and moderate renal impairment were 25 and 63% lower, respectively, than those in T2DM patients with normal renal function. These results are consistent with the observed clinical data from a previous renal impairment study.
Empirical models established based on the effect of UGE well predicted the renal function-dependent long-term glucose-lowering effects of ipragliflozin in patients with T2DM.
钠-葡萄糖协同转运蛋白2(SGLT2)抑制剂可抑制肾脏对葡萄糖的重吸收,增加尿糖排泄(UGE),从而降低1型和2型糖尿病(T2DM)患者的血糖浓度。在之前的一项研究中,我们报告了一个药代动力学/药效学模型,用于估计UGE的个体变化(ΔUGE),这是SGLT2抑制剂的直接药理作用。在本研究中,我们报告了对先前模型的改进,以预测依帕列净对T2DM患者临床结局的长期影响。
使用经验模型结合最大药物效应(E)模型和疾病进展模型,对早期临床试验中观察到的T2DM患者在接受依帕列净治疗后的空腹血糖(FPG)和糖化血红蛋白(HbA1c)的时间进程进行建模。作为药物效应的预测因子,将估计的ΔUGE引入E模型,而不是依帕列净暴露量。所建立的模型用于模拟安慰剂或依帕列净12.5、25、50和100mg剂量每日一次治疗后FPG和HbA1c的时间进程,并按肾功能类别总结在批准剂量50mg下52周时的变化。
发现以UGE作为反应因变量的所建立模型能够很好地描述观察到的FPG和HbA1c的时间进程。基线血糖水平和肾功能对依帕列净的降糖效果有显著影响,这些模型能够量化这些对临床结局的影响。轻度和中度肾功能损害的T2DM患者中,HbA1c的模拟中位数变化分别比肾功能正常的T2DM患者低25%和63%。这些结果与先前肾功能损害研究中观察到的临床数据一致。
基于UGE效应建立的经验模型很好地预测了依帕列净对T2DM患者肾功能依赖的长期降糖效果。
Zotero 插件
