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Application of Modeling and Simulation to a Long-Term Clinical Trial: A Direct Comparison of Simulated Data and Data Actually Observed in Japanese Osteoporosis Patients Following 3-Year Ibandronate Treatment

机译:建模和模拟在长期临床试验中的应用:模拟数据与日本伊波膦酸盐治疗3年后日本骨质疏松患者的实际观察结果的直接比较

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摘要

Ibandronate, a nitrogen-containing bisphosphonate, is a bone resorption inhibitor widely used to prevent and treat osteoporosis. To optimize the design for a long-term clinical study of ibandronate, modeling and simulation (M&S) was performed based on the result of population pharmacodynamic analysis using the data of a short-term clinical study. A population pharmacodynamic model was constructed by the urinary C-terminal telopeptide of type I collagen (uCTx) and the lumbar spine bone mineral density (BMD) data obtained in clinical studies, including a phase II study of Japanese osteoporosis patients treated with ibandronate for 6 months. Changes in BMD over a period of 3 years were simulated from the population pharmacodynamic parameters of the patients in this phase II study. The relationship between uCTx and BMD was well described by this modeling. The functions of disease progression and supplemental treatment were incorporated into the model to simulate a long-term clinical study with high accuracy. A long-term clinical study with a 3-year treatment was conducted after this M&S. The percentage change from baseline in observed BMD values were found to be similar to the prospectively simulated values. This study showed that M&S could be a useful and powerful tool for designing and conducting long-term clinical studies when carried out in the following sequence: (1) conduct a short-term clinical study; (2) perform M & S; and (3) conduct the long-term clinical study. Application of this procedure to various other treatment agents will establish the usefulness of M&S for long-term clinical studies and bring further efficiencies to drug development.
机译:伊班膦酸盐(一种含氮的双膦酸盐)是一种广泛用于预防和治疗骨质疏松症的骨吸收抑制剂。为了优化伊班膦酸的长期临床研究的设计,基于群体药效学分析的结果,使用短期临床研究的数据,进行了建模和仿真(M&S)。通过I型胶原的尿C端端端肽(uCTx)和临床研究中获得的腰椎骨矿物质密度(BMD)数据,建立了群体药效学模型,其中包括用伊班膦酸治疗6的日本骨质疏松症患者的II期研究个月。根据该II期研究中患者的总体药效学参数,模拟了3年内BMD的变化。该模型很好地描述了uCTx和BMD之间的关系。将疾病进展和补充治疗的功能纳入模型,以高精度模拟长期临床研究。在这次M&S之后,进行了为期3年的长期临床研究。发现观察到的BMD值相对于基线的百分比变化与预期模拟值相似。这项研究表明,按以下顺序进行,M&S可能是设计和进行长期临床研究的有用而强大的工具:(1)进行短期临床研究; (2)进行M&S; (3)进行长期临床研究。将该程序应用于其他各种治疗药物将建立M&S在长期临床研究中的有用性,并为药物开发带来更高的效率。

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