Orphanet Journal of Rare Diseases | |
A methodological framework for drug development in rare diseases | |
Catherine Cornu1  Behrouz Kassai1  Nathalie Eymard4  Vitaly Volpert4  Sylvie Chabaud3  Charlotte Castellan2  Salma Malik1  Agathe Bajard3  Polina Kurbatova4  Patrice Nony5  | |
[1] Hôpital Louis Pradel, Centre d¿Investigation Clinique, INSERM CIC1407/UMR5558, Bron, France;University of Lyon 1, UMR 5558, CNRS, Lyon, France;Unité de Biostatistique et d¿Evaluation des Thérapeutiques, Centre Léon Bérard, Lyon, France;Institut Camille Jordan UMR 5208 Université Claude Bernard, Lyon 1, France;Service de Pharmacologie Clinique et Essais Thérapeutiques-HCL, Groupement Hospitalier Est, Hôpital Cardiovasculaire et Pneumologique Louis Pradel, 28, Avenue du Doyen Lépine, Bron Cedex, 69677, France | |
关键词: Clinical trial simulation; Integrative modeling; Drug development; Rare diseases; | |
Others : 1149380 DOI : 10.1186/s13023-014-0164-y |
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received in 2014-06-02, accepted in 2014-10-14, 发布年份 2014 | |
【 摘 要 】
Introduction
Developing orphan drugs is challenging because of their severity and the requisite for effective drugs. The small number of patients does not allow conducting adequately powered randomized controlled trials (RCTs). There is a need to develop high quality, ethically investigated, and appropriately authorized medicines, without subjecting patients to unnecessary trials.
Aims and Objectives
The main aim is to develop generalizable framework for choosing the best-performing drug/endpoint/design combinations in orphan drug development using an in silico modeling and trial simulation approach. The two main objectives were (i) to provide a global strategy for each disease to identify the most relevant drugs to be evaluated in specific patients during phase III RCTs, (ii) and select the best design for each drug to be used in future RCTs.
Methodological approach
In silico phase III RCT simulation will be used to find the optimal trial design and was carried out in two steps: (i) statistical analysis of available clinical databases and (ii) integrative modeling that combines mathematical models for diseases with pharmacokinetic-pharmacodynamics models for the selected drug candidates.
Conclusion
There is a need to speed up the process of orphan drug development, develop new methods for translational research and personalized medicine, and contribute to European Medicines Agency guidelines. The approach presented here offers many perspectives in clinical trial conception.
【 授权许可】
2014 Nony et al.; licensee BioMed Central Ltd.
【 预 览 】
Files | Size | Format | View |
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20150405055057617.pdf | 770KB | download | |
Figure 2. | 134KB | Image | download |
Figure 1. | 33KB | Image | download |
【 图 表 】
Figure 1.
Figure 2.
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