We address the issue of analysis of clinical data generated by the bridging study conducted in the new region to evaluate the similarity for extrapolation of the foreign clinical data. A bridging study is usually conducted in the new region only after the test product is approved for commercial marketing in the original region due to its proven efficacy and safety. Sufficient information on efficacy, safety, dosage, and dose regimen has already generated in the original region. The empirical Bayesian approach is proposed to synthesize the data generated by the bridging study and foreign clinical data generated in the original region for assessment of similarity between the new and the original regions. A method for sample size determination for the bridging study is also suggested. It can be shown that the total sample size is inversely proportional to the strength of the evidence for the efficacy presented in the original region and the proportion of the patients assigned to receive the test product in the bridging study. *The views expressed in this article are personal opinions of the authors and may not necessarily represent the position of the National Cheng-Kung University, the National Health Research Institutes, and the National Cheng-Chi University, Taiwan.
[1]
S. Chow,et al.
Reproducibility probability in clinical trials
,
2002,
Statistics in medicine.
[2]
W. Shih,et al.
Clinical trials for drug registrations in Asian-Pacific countries: proposal for a new paradigm from a statistical perspective.
,
2001,
Controlled clinical trials.
[3]
James J. Chen,et al.
Sample Size Requirements for Evaluation of Bridging Evidence
,
2002
.
[4]
L. Joseph,et al.
Bayesian sample size determination for normal means and differences between normal means
,
1997
.
[5]
Shein-Chung Chow,et al.
ASSESSING SENSITIVITY AND SIMILARITY IN BRIDGING STUDIES
,
2002,
Journal of biopharmaceutical statistics.