Literature DB >> 20872623

Assessing consistent treatment effect in a multi-regional clinical trial: a systematic review.

Joshua Chen1, Hui Quan, Bruce Binkowitz, S Peter Ouyang, Yoko Tanaka, Gang Li, Shailendra Menjoge, Ekopimo Ibia.   

Abstract

A key issue in multi-regional clinical trials (MRCTs) is how to assess the consistency of treatment effect across regions, although there is no a priori reason to believe that the treatment effect should vary across the regions. In this article, we define the research question as an assessment of overall consistency across all regions for which all regions are considered equally important. This is different from the region/country-specific analyses (e.g. US vs Non-US), which are frequently requested by local regulatory agencies and usually performed for multiple agencies. We provide a systematic review of methods that may potentially be used for assessing consistency across regions, including commonly used quantitative/qualitative interaction tests, Japanese Pharmaceutical Medical Device Agency (PMDA) Methods 1 & 2, and those proposed for different purposes (e.g. bridging studies, meta-analysis, and vaccine lot consistency, among others). These methods are classified into three groups: global methods, multivariate quantitative methods, and multivariate qualitative methods. A case study is used to illustrate these methods. We also provide recommendations on how to choose appropriate methods and incorporate them in the study design.
Copyright © 2010 John Wiley & Sons, Ltd.

Mesh:

Year:  2010        PMID: 20872623     DOI: 10.1002/pst.438

Source DB:  PubMed          Journal:  Pharm Stat        ISSN: 1539-1604            Impact factor:   1.894


  1 in total

1.  Statistical design of noninferiority multiple region clinical trials to assess global and consistent treatment effects.

Authors:  Guoqing Diao; Donglin Zeng; Joseph G Ibrahim; Alan Rong; Oliver Lee; Kathy Zhang; Qingxia Chen
Journal:  J Biopharm Stat       Date:  2017-03-15       Impact factor: 1.051

  1 in total

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