Trial designs using real‐world data: The changing landscape of the regulatory approval process

Andre, Elodie Baumfeld; Reynolds, Robert F.; Caubel, Patrick; Azoulay, Laurent; Dreyer, Nancy A

doi:10.1002/pds.4932

Cited by 159 publications

(141 citation statements)

References 30 publications

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“…It is at this juncture that the healthcare industry is now recognising the potential of RWD as a source of clinically meaningful evidence for consideration by key industry decision-makers, including when embedded within traditional RCT assessments [ 5 , 6 ]. The value of RWE is attributed to the fact that data collection is undertaken for routine care and practice, making RWD creation essentially free of charge with the added benefit of being representative of typical patients, events and outcomes.…”

Section: Introductionmentioning

confidence: 99%

Bridging the Gap Between RCTs and RWE Through Endpoint Selection

LoCasale

Pashos

Gutierrez

et al. 2020

Ther Innov Regul Sci

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This commentary is authored by several industry real-world evidence (RWE) experts, with support from IQVIA, as part of the 'RWE Leadership Forum': a group of Industry Leaders who have come together as non-competitive partners to understand and respond to RWD/E challenges and opportunities with a single expert voice. Here, the forum discusses the value in bridging the industry disconnect between RTCs and RWE, with a view to promoting the use of RWE in the RCT environment. RCT endpoints are explored along several axes including their clinical relevance and their measure of direct patient benefit, and then compared with their real-world counterparts to identify suitable paths, or gaps, for assimilating RWE endpoints into the RCT environment.

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Section: Introductionmentioning

confidence: 99%

Bridging the Gap Between RCTs and RWE Through Endpoint Selection

LoCasale

Pashos

Gutierrez

et al. 2020

Ther Innov Regul Sci

Self Cite

View full text Add to dashboard Cite

show abstract

“…20 From a regulatory perspective, RWE may now be used to support label expansion (including new indications, dosages, and patient sub-populations), to assess the feasibility of Phase IV studies, to provide evidence for products in an expedited approval pathway, to provide a historical control arm for clinical studies, and in pragmatic trials. 5 Indeed, there is a growing list of drug approvals and labelling changes that have utilized RWE and data from nontraditional study designs in their regulatory submissions. 21 For example, an expansion in the indication of palbociclib was supported by RWD from EHR and insurance claims.…”

Section: Rwe For Regulatory Purposesmentioning

confidence: 99%

“…4 RWE may be generated from different study designs or analyses, including randomized (non-controlled) trials, large simple trials, pragmatic trials (ie, trials that incorporate elements of routine clinical practice), and prospective or retrospective observational studies. 5 RWE can be derived from a variety of sources. Therefore, its use provides an opportunity to combine diverse datasets to provide a broader understanding than might be available through RCTs.…”

Section: Introductionmentioning

confidence: 99%

<p>Harnessing Real-World Data for Regulatory Use and Applying Innovative Applications</p>

Zou¹,

Li²,

Imperato³

et al. 2020

JMDH

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A vast quantity of real-world data (RWD) are available to healthcare researchers. Such data come from diverse sources such as electronic health records, insurance claims and billing activity, product and disease registries, medical devices used in the home, and applications on mobile devices. The analysis of RWD produces real-world evidence (RWE), which is clinical evidence that provides information about usage and potential benefits or risks of a drug. This review defines and explains RWD, and it also details how regulatory authorities are using RWD and RWE. The main challenges in harnessing RWD include collating and analyzing numerous disparate types or categories of available information including both structured (eg, field entries) and unstructured (eg, doctor notes, discharge summaries, social media posts) data. Although the use of artificial intelligence to capture, amalgamate, standardize, and analyze RWD is still evolving, it has the potential to support the increased use of RWE to improve global health and healthcare.

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“…Initial regulatory approval of novel oncology compounds could be based on such a single-arm trial [1,2]. However, to provide additional context to regulators, the sponsor has decided to construct an external control arm for the trial, using data retrospectively collected from an electronic health records system [3,4]. The sponsor will compare overall survival for patients in the external control arm to overall survival for patients in the single-arm trial, after reweighting to account for differences in patient characteristics.…”

Section: Introductionmentioning

confidence: 99%

How to choose a time zero for patients in external control arms

Backenroth

2020

Preprint

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When a sponsor carries out a single-arm trial of a novel oncology compound, it may wish to assess the efficacy of the compound via comparison of overall survival to an external control arm, constructed using patients included in some retrospective registry. If efficacy of the novel compound is compared to efficacy of physician’s choice of chemotherapy, patients in the retrospective registry might qualify for inclusion in the external control arm at multiple different points in time, when they receive different chemotherapy treatments. For example, a patient might qualify at the start of their second, third and fourth lines of therapy. From the start of which line of therapy should this patient’s survival be compared to survival of participants in the single-arm trial?Some sponsors have elected to include patients in the external control arm from the last available line of therapy in the retrospective database. Another possibility is to randomly select a line of therapy for each external control arm patient from among those available. In this paper, we show, via probabilistic arguments and also via simulation based on real data, that both of these methods give rise to a bias in favor of the single-arm trial. We further show that this bias can be avoided by instead including external control arm patients multiple times in the external control arm, once for each time they receive qualifying treatment.

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Trial designs using real‐world data: The changing landscape of the regulatory approval process

Cited by 159 publications

References 30 publications

Bridging the Gap Between RCTs and RWE Through Endpoint Selection

Bridging the Gap Between RCTs and RWE Through Endpoint Selection

<p>Harnessing Real-World Data for Regulatory Use and Applying Innovative Applications</p>

How to choose a time zero for patients in external control arms

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