Seamless Designs: Current Practice and Considerations for Early-Phase Drug Development in Oncology

Hobbs, Brian P.; Barata, Pedro C.; Kanjanapan, Yada; Paller, Channing J.; Perlmutter, Jane; Pond, Gregory R.; Prowell, Tatiana M.; Rubin, Eric H.; Seymour, Lesley; Wages, Nolan A.; Yap, Timothy A.; Feltquate, David; Garrett‐Mayer, Elizabeth; Grossman, William; Hong, David S.; Ivy, S. Percy; Siu, Lillian L.; Reeves, Steven A.; Rosner, Gary L.

doi:10.1093/jnci/djy196

Cited by 54 publications

(47 citation statements)

References 72 publications

(38 reference statements)

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“…The traditional paradigm of drug development in malignancies is a sequential evaluation of efficacy and safety, from primary safety evaluation in phase I and first-in-human studies, to be followed by dose finding and preliminary efficacy studies in phase II. 1 When successful, these exploratory findings in patients with advanced disease would then lead to confirmation of clinical efficacy and safety, and benefits relative to the existing, best available standard-of-care, in a randomized phase III clinical trial. Generally, randomized clinical trials are also recommended by the European Medicines Agency (EMA) anticancer guideline and have been considered a way to obtain high-quality data for clinicans and patients to make informed treatment decisions, and to faciliate evidence-based global access to new anticancer products.…”

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confidence: 98%

“…Generally, randomized clinical trials are also recommended by the European Medicines Agency (EMA) anticancer guideline and have been considered a way to obtain high-quality data for clinicans and patients to make informed treatment decisions, and to faciliate evidence-based global access to new anticancer products. [1][2][3] Advances in molecular biology and immunology have refined and challenged our understanding of cancer biology and new therapeutic targets for anticancer products. 2 Leading to concepts of personalized cancer therapy, targeted agents, and precision oncology, these findings have had multiple consequences on the evolution of clinical study designs.…”

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confidence: 99%

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Single‐Arm Clinical Trials as Pivotal Evidence for Cancer Drug Approval: A Retrospective Cohort Study of Centralized European Marketing Authorizations Between 2010 and 2019

Tenhunen

Lasch

Schiel

et al. 2020

Clin Pharma and Therapeutics

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The traditional drug development paradigm, consisting of sequential phases and randomized studies, has been challenged in oncology and hemato‐oncology. In the regulatory context, a number of new products have been authorized based on nonrandomized efficacy and safety data. We retrospectively analyzed the European public assessment reports for anticancer treatments authorized between 2010 and 2019 to describe the data behind such approvals. Twenty‐two initial marketing authorizations, mainly conditional, were identified. Fifty percent of the products had an orphan indication, and 77% had received previous scientific advice. Conclusions of clinical benefit were based on tumor responses, ranging between 15.8 and 88%. Our data shows that single‐arm clinical studies leading to positive regulatory outcomes share common methodological approaches and end points, mostly comparing the overall response rate with a fixed success threshold as the primary analysis. The clinical indications in these approvals are clustered in late‐line settings, hematological malignancies, and lung cancer. Our findings underline the need to reflect on the current practice, the methodological aspects, and end points in single‐arm studies, and develop specific regulatory guidance on nonrandomized and novel study designs.

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confidence: 98%

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confidence: 99%

Single‐Arm Clinical Trials as Pivotal Evidence for Cancer Drug Approval: A Retrospective Cohort Study of Centralized European Marketing Authorizations Between 2010 and 2019

Tenhunen

Lasch

Schiel

et al. 2020

Clin Pharma and Therapeutics

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“…37 The incorporation of a biomarker-based strategy in drug development timelines for new oncology drugs has been reported to reduce the time to approval. 38 Unfortunately, this could not be analyzed as the non-personalized carfilzomib was the only common CDP. Innovative concepts related to the Phase I program have also been debated but not analyzed.…”

Section: Discussionmentioning

confidence: 99%

<p>The European Medicines Agency Clinical Data Website Enables Insights Into Clinical Development Timelines And Strategy</p>

Lehmann¹,

Allard²,

Boehler³

2019

OAJCT

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Purpose: The clinical study report (CSR) documents of a full clinical development pathway (CDP) have been publicly available on the European Medicines Agency (EMA; Amsterdam, Netherlands) clinical data website (ECDW) since October 2016. Our analysis aimed to determine the extent to which the available clinical development program could be assessed. Methods: The documents available on the ECDW up to April 1, 2018 and the corresponding European Public Assessment Report (EPAR) were reviewed. Information extracted from the available CSRs focused on dates, phase of development, module leaf structure, and number of protocol amendments. Data analyses included generalized activity normalization time table (GANTT) charts and network analyses. Results: Of the 86 available CDPs, 55 were initial marketing authorizations covering a diverse range of clinical developments from generics to advanced therapy in the electronic common technical documents (eCTDs). Non-redacted dates were available in 444 CSRs from 15 CDPs to perform retrospective project clinical development management analyses. In these 15 marketing authorizations, the median timespan to submission was 9.3 years (range: 6.2-22.2). The timespan within these 15 clinical developments ranged from 5.9 to 21.4 years (median 8.3). The median time to first-subject-in in the first controlled clinical study pertinent to the claimed indication (CCSPCI) was 4.4 years (range: 0-12.1); the duration of the CCSPCI ranged from 2.4 to 16.9 years (median: 4.4; interquartile range: 4.2-7.0). Four CDPs had concurrent subject enrolment, while seven CDPs had seamless study designs. Subject participation ranged from 52% to 97% of a clinical development timeline. Conclusion: The publication of CSR documents by the EMA has enabled insights into timelines and project management aspects of the clinical development of medications.

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“…This may take the path of the traditional paradigm of distinctive trial phases or morph to seamless or tissue-agnostic designs to speed up subsequent steps. Regardless of the strategy, investigators must comply with established scientific, ethical, and biostatistical principles and standards to ensure data integrity and study subject protection (27).…”

Section: Phase I-iii Paradigm: What Needs To Stay What Needs To Go?mentioning

confidence: 99%

The Future of Clinical Trial Design in Oncology

et al. 2021

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Clinical trials represent a fulcrum for oncology drug discovery and development to bring safe and effective medicines to patients in a timely manner. Clinical trials have shifted from traditional studies evaluating cytotoxic chemotherapy in largely histology-based populations to become adaptively designed and biomarker-driven evaluations of molecularly targeted agents and immune therapies in selected patient subsets. This review will discuss the scientific, methodological, practical, and patient-focused considerations to transform clinical trials. A call to action is proposed to establish the framework for next-generation clinical trials that strikes an optimal balance of operational efficiency, scientific impact, and value to patients.Research.

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Seamless Designs: Current Practice and Considerations for Early-Phase Drug Development in Oncology

Cited by 54 publications

References 72 publications

Single‐Arm Clinical Trials as Pivotal Evidence for Cancer Drug Approval: A Retrospective Cohort Study of Centralized European Marketing Authorizations Between 2010 and 2019

Single‐Arm Clinical Trials as Pivotal Evidence for Cancer Drug Approval: A Retrospective Cohort Study of Centralized European Marketing Authorizations Between 2010 and 2019

<p>The European Medicines Agency Clinical Data Website Enables Insights Into Clinical Development Timelines And Strategy</p>

The Future of Clinical Trial Design in Oncology

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