Advanced methods for dose and regimen finding during drug development: Summary of the EMA/EFPIA workshop on dose finding (London 4-5 December 2014)

Flora Musuamba Tshinanu; E. Manolis; N. Holford; S. Y.A. Cheung; L. E. Friberg; K. Ogungbenro; M. Posch; J. W.T. Yates; S. Berry; N. Thomas; S. Corriol-Rohou; B. Bornkamp; F. Bretz; A. C. Hooker; P. H. Van Der Graaf; J. F. Standing; J. Hay; S. Cole; V. Gigante; K. Karlsson; T. Dumortier; N. Benda; F. Serone; S. Das; A. Brochot; F. Ehmann; R. Hemmings; I. Skottheim Rusten

doi:10.1002/psp4.12196

Advanced methods for dose and regimen finding during drug development: Summary of the EMA/EFPIA workshop on dose finding (London 4-5 December 2014)

Flora Musuamba Tshinanu, E. Manolis, N. Holford, S. Y.A. Cheung, L. E. Friberg, K. Ogungbenro, M. Posch, J. W.T. Yates, S. Berry, N. Thomas, S. Corriol-Rohou, B. Bornkamp, F. Bretz, A. C. Hooker, P. H. Van Der Graaf, J. F. Standing, J. Hay, S. Cole, V. Gigante, K. KarlssonT. Dumortier, N. Benda, F. Serone, S. Das, A. Brochot, F. Ehmann, R. Hemmings, I. Skottheim Rusten

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Abstract

Inadequate dose selection for confirmatory trials is currently still one of the most challenging issues in drug development, as illustrated by high rates of late-stage attritions in clinical development and postmarketing commitments required by regulatory institutions. In an effort to shift the current paradigm in dose and regimen selection and highlight the availability and usefulness of well-established and regulatory-acceptable methods, the European Medicines Agency (EMA) in collaboration with the European Federation of Pharmaceutical Industries Association (EFPIA) hosted a multistakeholder workshop on dose finding (London 4-5 December 2014). Some methodologies that could constitute a toolkit for drug developers and regulators were presented. These methods are described in the present report: they include five advanced methods for data analysis (empirical regression models, pharmacometrics models, quantitative systems pharmacology models, MCP-Mod, and model averaging) and three methods for study design optimization (Fisher information matrix (FIM)-based methods, clinical trial simulations, and adaptive studies). Pairwise comparisons were also discussed during the workshop; however, mostly for historical reasons. This paper discusses the added value and limitations of these methods as well as challenges for their implementation. Some applications in different therapeutic areas are also summarized, in line with the discussions at the workshop. There was agreement at the workshop on the fact that selection of dose for phase III is an estimation problem and should not be addressed via hypothesis testing. Dose selection for phase III trials should be informed by well-designed dosefinding studies; however, the specific choice of method(s) will depend on several aspects and it is not possible to recommend a generalized decision tree. There are many valuable methods available, the methods are not mutually exclusive, and they should be used in conjunction to ensure a scientifically rigorous understanding of the dosing rationale.

Original language	English
Pages (from-to)	418-429
Number of pages	12
Journal	CPT: Pharmacometrics and Systems Pharmacology
Volume	6
Issue number	7
DOIs	https://doi.org/10.1002/psp4.12196
Publication status	Published - Jul 2017
Externally published	Yes

Funding

Funders	Funder number
European Commission
Seventh Framework Programme	603160
Medical Research Council	MR/M008665/1

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CPT Pharmacom Syst Pharma - 2017 - Musuamba - Advanced Methods for Dose and Regimen Finding During Drug Development Final published version, 234 KB

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Musuamba Tshinanu, F., Manolis, E., Holford, N., Cheung, S. Y. A., Friberg, L. E., Ogungbenro, K., Posch, M., Yates, J. W. T., Berry, S., Thomas, N., Corriol-Rohou, S., Bornkamp, B., Bretz, F., Hooker, A. C., Van Der Graaf, P. H., Standing, J. F., Hay, J., Cole, S., Gigante, V., ... Skottheim Rusten, I. (2017). Advanced methods for dose and regimen finding during drug development: Summary of the EMA/EFPIA workshop on dose finding (London 4-5 December 2014). CPT: Pharmacometrics and Systems Pharmacology, 6(7), 418-429. https://doi.org/10.1002/psp4.12196

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title = "Advanced methods for dose and regimen finding during drug development: Summary of the EMA/EFPIA workshop on dose finding (London 4-5 December 2014)",

abstract = "Inadequate dose selection for confirmatory trials is currently still one of the most challenging issues in drug development, as illustrated by high rates of late-stage attritions in clinical development and postmarketing commitments required by regulatory institutions. In an effort to shift the current paradigm in dose and regimen selection and highlight the availability and usefulness of well-established and regulatory-acceptable methods, the European Medicines Agency (EMA) in collaboration with the European Federation of Pharmaceutical Industries Association (EFPIA) hosted a multistakeholder workshop on dose finding (London 4-5 December 2014). Some methodologies that could constitute a toolkit for drug developers and regulators were presented. These methods are described in the present report: they include five advanced methods for data analysis (empirical regression models, pharmacometrics models, quantitative systems pharmacology models, MCP-Mod, and model averaging) and three methods for study design optimization (Fisher information matrix (FIM)-based methods, clinical trial simulations, and adaptive studies). Pairwise comparisons were also discussed during the workshop; however, mostly for historical reasons. This paper discusses the added value and limitations of these methods as well as challenges for their implementation. Some applications in different therapeutic areas are also summarized, in line with the discussions at the workshop. There was agreement at the workshop on the fact that selection of dose for phase III is an estimation problem and should not be addressed via hypothesis testing. Dose selection for phase III trials should be informed by well-designed dosefinding studies; however, the specific choice of method(s) will depend on several aspects and it is not possible to recommend a generalized decision tree. There are many valuable methods available, the methods are not mutually exclusive, and they should be used in conjunction to ensure a scientifically rigorous understanding of the dosing rationale.",

author = "\{Musuamba Tshinanu\}, Flora and E. Manolis and N. Holford and Cheung, \{S. Y.A.\} and Friberg, \{L. E.\} and K. Ogungbenro and M. Posch and Yates, \{J. W.T.\} and S. Berry and N. Thomas and S. Corriol-Rohou and B. Bornkamp and F. Bretz and Hooker, \{A. C.\} and \{Van Der Graaf\}, \{P. H.\} and Standing, \{J. F.\} and J. Hay and S. Cole and V. Gigante and K. Karlsson and T. Dumortier and N. Benda and F. Serone and S. Das and A. Brochot and F. Ehmann and R. Hemmings and \{Skottheim Rusten\}, I.",

year = "2017",

month = jul,

doi = "10.1002/psp4.12196",

language = "English",

volume = "6",

pages = "418--429",

journal = "CPT: Pharmacometrics and Systems Pharmacology",

publisher = "American Society for Clinical Pharmacology and Therapeutics",

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Musuamba Tshinanu, F, Manolis, E, Holford, N, Cheung, SYA, Friberg, LE, Ogungbenro, K, Posch, M, Yates, JWT, Berry, S, Thomas, N, Corriol-Rohou, S, Bornkamp, B, Bretz, F, Hooker, AC, Van Der Graaf, PH, Standing, JF, Hay, J, Cole, S, Gigante, V, Karlsson, K, Dumortier, T, Benda, N, Serone, F, Das, S, Brochot, A, Ehmann, F, Hemmings, R & Skottheim Rusten, I 2017, 'Advanced methods for dose and regimen finding during drug development: Summary of the EMA/EFPIA workshop on dose finding (London 4-5 December 2014)', CPT: Pharmacometrics and Systems Pharmacology, vol. 6, no. 7, pp. 418-429. https://doi.org/10.1002/psp4.12196

TY - JOUR

T1 - Advanced methods for dose and regimen finding during drug development

T2 - Summary of the EMA/EFPIA workshop on dose finding (London 4-5 December 2014)

AU - Musuamba Tshinanu, Flora

AU - Manolis, E.

AU - Holford, N.

AU - Cheung, S. Y.A.

AU - Friberg, L. E.

AU - Ogungbenro, K.

AU - Posch, M.

AU - Yates, J. W.T.

AU - Berry, S.

AU - Thomas, N.

AU - Corriol-Rohou, S.

AU - Bornkamp, B.

AU - Bretz, F.

AU - Hooker, A. C.

AU - Van Der Graaf, P. H.

AU - Standing, J. F.

AU - Hay, J.

AU - Cole, S.

AU - Gigante, V.

AU - Karlsson, K.

AU - Dumortier, T.

AU - Benda, N.

AU - Serone, F.

AU - Das, S.

AU - Brochot, A.

AU - Ehmann, F.

AU - Hemmings, R.

AU - Skottheim Rusten, I.

PY - 2017/7

Y1 - 2017/7

N2 - Inadequate dose selection for confirmatory trials is currently still one of the most challenging issues in drug development, as illustrated by high rates of late-stage attritions in clinical development and postmarketing commitments required by regulatory institutions. In an effort to shift the current paradigm in dose and regimen selection and highlight the availability and usefulness of well-established and regulatory-acceptable methods, the European Medicines Agency (EMA) in collaboration with the European Federation of Pharmaceutical Industries Association (EFPIA) hosted a multistakeholder workshop on dose finding (London 4-5 December 2014). Some methodologies that could constitute a toolkit for drug developers and regulators were presented. These methods are described in the present report: they include five advanced methods for data analysis (empirical regression models, pharmacometrics models, quantitative systems pharmacology models, MCP-Mod, and model averaging) and three methods for study design optimization (Fisher information matrix (FIM)-based methods, clinical trial simulations, and adaptive studies). Pairwise comparisons were also discussed during the workshop; however, mostly for historical reasons. This paper discusses the added value and limitations of these methods as well as challenges for their implementation. Some applications in different therapeutic areas are also summarized, in line with the discussions at the workshop. There was agreement at the workshop on the fact that selection of dose for phase III is an estimation problem and should not be addressed via hypothesis testing. Dose selection for phase III trials should be informed by well-designed dosefinding studies; however, the specific choice of method(s) will depend on several aspects and it is not possible to recommend a generalized decision tree. There are many valuable methods available, the methods are not mutually exclusive, and they should be used in conjunction to ensure a scientifically rigorous understanding of the dosing rationale.

AB - Inadequate dose selection for confirmatory trials is currently still one of the most challenging issues in drug development, as illustrated by high rates of late-stage attritions in clinical development and postmarketing commitments required by regulatory institutions. In an effort to shift the current paradigm in dose and regimen selection and highlight the availability and usefulness of well-established and regulatory-acceptable methods, the European Medicines Agency (EMA) in collaboration with the European Federation of Pharmaceutical Industries Association (EFPIA) hosted a multistakeholder workshop on dose finding (London 4-5 December 2014). Some methodologies that could constitute a toolkit for drug developers and regulators were presented. These methods are described in the present report: they include five advanced methods for data analysis (empirical regression models, pharmacometrics models, quantitative systems pharmacology models, MCP-Mod, and model averaging) and three methods for study design optimization (Fisher information matrix (FIM)-based methods, clinical trial simulations, and adaptive studies). Pairwise comparisons were also discussed during the workshop; however, mostly for historical reasons. This paper discusses the added value and limitations of these methods as well as challenges for their implementation. Some applications in different therapeutic areas are also summarized, in line with the discussions at the workshop. There was agreement at the workshop on the fact that selection of dose for phase III is an estimation problem and should not be addressed via hypothesis testing. Dose selection for phase III trials should be informed by well-designed dosefinding studies; however, the specific choice of method(s) will depend on several aspects and it is not possible to recommend a generalized decision tree. There are many valuable methods available, the methods are not mutually exclusive, and they should be used in conjunction to ensure a scientifically rigorous understanding of the dosing rationale.

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ER -

Advanced methods for dose and regimen finding during drug development: Summary of the EMA/EFPIA workshop on dose finding (London 4-5 December 2014)

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