A case study: Assessing the efficacy of the revised dosage regimen via prediction model for recurrent event rate using biomarker data.

IF 1.3 4区 医学 Q4 PHARMACOLOGY & PHARMACY
Pharmaceutical Statistics Pub Date : 2024-07-01 Epub Date: 2024-02-05 DOI:10.1002/pst.2362
Ahrim Youn, Jiarui Chi, Yue Cui, Hui Quan
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引用次数: 0

Abstract

In recently conducted phase III trials in a rare disease area, patients received monthly treatment at a high dose of the drug, which targets to lower a specific biomarker level, closely associated with the efficacy endpoint, to around 10% across patients. Although this high dose demonstrated strong efficacy, treatments were withheld due to the reports of serious adverse events. Dosing in these studies were later resumed at a reduced dosage which targets to lower the biomarker level to 15%-35% across patients. Two questions arose after this disruption. The first is whether the efficacy of this revised regimen as measured by the reduction in annualized event rate is adequate to support the continuation of the development and the second is whether the potential bias due to the loss of patients during this dosing gap process can be gauged. To address these questions, we built a prediction model that quantitatively characterizes biomarker vs. endpoint relationship and predicts efficacy at the 15%-35% range of the biomarker level using the available data from the original high dose. This model predicts favorable event rate in the target biomarker level and shows that the bias due to the loss of patients is limited. These results support the continued development of the revised regimen, however, given the limitation of the data available, this prediction is planned to be validated further when data under the revised regimen become available.

案例研究:利用生物标志物数据建立复发率预测模型,评估修订剂量方案的疗效。
最近在一个罕见病领域开展的 III 期试验中,患者每月接受一次高剂量药物治疗,目标是将与疗效终点密切相关的特定生物标志物水平降至患者的 10%左右。虽然这种高剂量药物显示出很强的疗效,但由于出现了严重的不良反应,治疗被迫中止。后来,这些研究恢复了减量给药,目标是将患者的生物标志物水平降至 15%-35%。这次中断后出现了两个问题。第一个问题是,根据年化事件发生率的降低程度来衡量,这一修订方案的疗效是否足以支持继续开发;第二个问题是,是否可以衡量在这一剂量间隙过程中因患者流失而产生的潜在偏差。为了解决这些问题,我们建立了一个预测模型,定量描述生物标志物与终点的关系,并利用原始高剂量的可用数据预测生物标志物水平在 15%-35% 范围内的疗效。该模型预测了目标生物标志物水平的有利事件发生率,并表明由于患者流失造成的偏差是有限的。这些结果支持继续开发修订后的治疗方案,但鉴于现有数据的局限性,计划在获得修订后治疗方案的数据后进一步验证这一预测。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Pharmaceutical Statistics
Pharmaceutical Statistics 医学-统计学与概率论
CiteScore
2.70
自引率
6.70%
发文量
90
审稿时长
6-12 weeks
期刊介绍: Pharmaceutical Statistics is an industry-led initiative, tackling real problems in statistical applications. The Journal publishes papers that share experiences in the practical application of statistics within the pharmaceutical industry. It covers all aspects of pharmaceutical statistical applications from discovery, through pre-clinical development, clinical development, post-marketing surveillance, consumer health, production, epidemiology, and health economics. The Journal is both international and multidisciplinary. It includes high quality practical papers, case studies and review papers.
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