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首页> 外文期刊>Saudi Pharmaceutical Journal >Utilization of model-based meta-analysis to delineate the net efficacy of taspoglutide from the response of placebo in clinical trials
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Utilization of model-based meta-analysis to delineate the net efficacy of taspoglutide from the response of placebo in clinical trials

机译:在临床试验中利用基于模型的荟萃分析从安慰剂反应中描绘出塔斯波鲁肽的净功效

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The objective of this study was to develop quantitative models to delineate the net efficacy of taspoglutide on fasting plasma glucose (FPG) and glycosylated hemoglobin (HbA1c) from the response of placebo in type 2 diabetes patients, and further find pharmacodynamic potency of taspoglutide and FPG for half of maximum reduction responses of FPG and HbA1c, respectively. Several PD data about taspoglutide treatments for type 2 diabetes patients were digitalized from the published papers related with the clinical development of taspoglutide. The model based meta-analysis (MBMA) studies for FPG and HbA1c were performed with Monolix 4.2 software. The MBMA successfully described the effects of placebo and taspoglutide on pharmacological indexes of FPG and HbA1c through mono and multiple combination therapies in clinical trials. The pharmacodynamic potency (25.3pmol/l) produced 50% of maximum responses of FPG (-2.39mmol/l) from the responses of placebo for FPG (-0.371mmol/l); the response change of FPG (-1.81mmol/l) affected 50% of maximum response change (-1.74%) for HbA1c from the response of placebo (-0.253%). The leveraging prior knowledge from the longitudinal MBMA will be utilized to guide clinical development of taspoglutide and further support study designs including optimization of dose and duration of therapy.
机译:这项研究的目的是建立定量模型,从安慰剂对2型糖尿病患者的反应中勾勒出塔斯波鲁肽对空腹血糖(FPG)和糖基化血红蛋白(HbA1c)的净功效,并进一步发现塔斯波鲁肽和FPG的药效学潜力FPG和HbA1c最大还原反应的一半。从有关他曲鲁肽临床开发的已发表论文中,数字化了有关他曲戊肽治疗2型糖尿病患者的几项PD数据。使用Monolix 4.2软件对FPG和HbA1c进行基于模型的荟萃分析(MBMA)研究。 MBMA在临床试验中通过单一和多种联合疗法成功地描述了安慰剂和他司鲁肽对FPG和HbA1c药理指标的影响。安慰剂对FPG的反应(-0.371mmol / l)的药效学效力(25.3pmol / l)产生了FPG最大反应(-2.39mmol / l)的50%; FPG(-1.81mmol / l)的响应变化影响了HbA1c的最大响应变化(-0.253%)的50%。来自纵向MBMA的先验知识将被用于指导taspoglutide的临床开发,并进一步支持研究设计,包括优化剂量和治疗持续时间。

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