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有界结局评分模型:在使用乌司奴单抗治疗银屑病中的应用。

Bounded outcome score modeling: application to treating psoriasis with ustekinumab.

机构信息

Pharmacokinetics and Pharmacometrics, Biologics Clinical Pharmacology, Centocor R&D, A Division of Johnson & Johnson Pharmaceutical Research & Development, LLC., Parkway, Malvern, PA 19355, USA.

出版信息

J Pharmacokinet Pharmacodyn. 2011 Aug;38(4):497-517. doi: 10.1007/s10928-011-9205-5. Epub 2011 Jun 18.

DOI:10.1007/s10928-011-9205-5
PMID:21688068
Abstract

Disease status is often measured with bounded outcome scores (BOS) which report a discrete set of values on a finite range. The distribution of BOS data is often non-standard, e.g., J- or U-shaped, thus making standard analysis methods that assume normality inappropriate. Data transformations aiming to achieve normality with BOS can be much more difficult than with many other types of skewed distributions, and application of methodologies explicitly dealing with this problem has not been previously published in pharmacokinetic/pharmacodynamic modeling literature. In this analysis, a coarsened latent variable (CO) approach is augmented with flexible transformations and applied for the purpose of demonstrating ustekinumab effects on four clinical components (involved body surface area, induration, erythema, and scaling) in patients with moderate to severe psoriasis from two Phase 3 studies. Patients were randomized to receive placebo or ustekinumab 45 or 90 mg, followed by randomized withdrawal and long-term extension periods. The approach was used together with a previously established novel semi-mechanistic, mixed-effect exposure-response model integrated with placebo effect and disease progression, and with potential influence of dropout investigated. An additional transformation further modifying both tails of the standard logit transformation in the original CO approach was shown to be necessary in this application.

摘要

疾病状况通常通过有界结局评分(BOS)进行衡量,BOS 在有限范围内报告一组离散的值。BOS 数据的分布通常是非标准的,例如 J 形或 U 形,因此,假设正态性的标准分析方法并不适用。与许多其他类型的偏态分布相比,BOS 数据的正态化转换可能更加困难,并且以前在药代动力学/药效学建模文献中没有发表过专门处理此问题的方法。在这项分析中,粗糙化潜在变量(CO)方法与灵活的转换相结合,用于从两项 3 期研究中展示乌司奴单抗对中重度银屑病患者的四个临床指标(受累体表面积、硬结、红斑和鳞屑)的影响。患者随机接受安慰剂或乌司奴单抗 45 或 90mg,随后进行随机停药和长期扩展期。该方法与之前建立的新型半机理、混合效应暴露-反应模型相结合,该模型与安慰剂效应和疾病进展相结合,并研究了脱落的潜在影响。在这种应用中,需要对原始 CO 方法中的标准对数转换的两个尾部进行进一步的转换修改。

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