Characteristics of Clinical Studies Conducted Over the Total Product Life Cycle of High-Risk Therapeutic Medical Devices Receiving FDA Premarket Approval in 2010 and 2011

Rathi, Vinay K.; Krumholz, Harlan M.; Masoudi, Frederick A.; Ross, Joseph S.

doi:10.1001/jama.2015.8761

Cited by 89 publications

(116 citation statements)

References 24 publications

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“…Our findings are consistent with previous studies showing that even postapproval studies required by the FDA to be conducted by manufacturers are not always performed in a timely manner [13][14][15] and with previous work demonstrating the variability in the number and completion of postmarketing studies of high risk medical devices. 25 The majority of the postapproval studies that we identified focused on surrogate markers of disease. Using surrogate markers instead of clinical outcomes for trial endpoints has become increasingly controversial, 26 with several approved drugs ultimately failing to confirm any clinical benefit [27][28][29] and an analysis of oncology surrogate markers finding variable correlation with overall survival.…”

Section: Discussionmentioning

confidence: 99%

Postapproval studies of drugs initially approved by the FDA on the basis of limited evidence: systematic review

Pease

Krumholz

Downing

et al. 2017

BMJ

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Objective To characterize the prospective controlled clinical studies for all novel drugs that were initially approved by the Food and Drug Administration on the basis of limited evidence. Design Systematic review. Data sources Drugs@FDA database and PubMed. Study inclusion All prospective controlled clinical studies published after approval for all novel drugs initially approved by the FDA between 2005 and 2012 on the basis of a single pivotal trial, pivotal trials that used surrogate markers of disease as primary endpoints, or both. Results Between 2005 and 2012 the FDA approved 117 novel drugs for 123 indications on the basis of a single pivotal trial, pivotal trials that used surrogate markers of disease, or both (single surrogate trials). We identified 758 published controlled studies over a median of 5.5 years (interquartile range 3.4-8.2) after approval, most of which (554 of 758; 73.1%) were studies for indications approved on the basis of surrogate markers of disease. Most postapproval studies used active comparators—67 of 77 (87.0%) indications approved on the basis of single pivotal trials, 365 of 554 (65.9%) approvals based on surrogate marker trials, and 100 of 127 (78.7%) approvals based on single surrogate trials—and examined surrogate markers of efficacy as primary endpoints—51 of 77 (66.2%), 512 of 554 (92.4%), and 110 of 127 (86.6%), respectively. Overall, no postapproval studies were identified for 43 of the 123 (35.0%) approved indications. The median total number of postapproval studies identified was 1 (interquartile range 0-2) for indications approved on the basis of a single pivotal trial, 3 (1-8) for indications approved on the basis of pivotal trials that used surrogate markers of disease as primary endpoints, and 1 (0-2) for single surrogate trial approvals, and the median aggregate number of patients enrolled in postapproval studies was 90 (0-509), 533 (122-3633), and 38 (0-666), respectively. The proportion of approved indications with one or more randomized, controlled, double blind study using a clinical outcome for the primary endpoint that was published after approval and showed superior efficacy was 18.2% (6 of 33), 2.0% (1 of 49), and 4.9% (2 of 41), respectively. Conclusions The quantity and quality of postapproval clinical evidence varied substantially for novel drugs first approved by the FDA on the basis of limited evidence, with few controlled studies published after approval that confirmed efficacy using clinical outcomes for the original FDA approved indication.

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Section: Discussionmentioning

confidence: 99%

Postapproval studies of drugs initially approved by the FDA on the basis of limited evidence: systematic review

Pease

Krumholz

Downing

et al. 2017

BMJ

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“…The FDA requires one pivotal and one non pivotal study for device approval, at minimum. A recent review of clinical trials found that the majority of devices have been approved with these minimal requirements, though some companies have ongoing studies throughout the device lifespan [7]. Regulatory bodies are left with the burden of navigating grey areas in approval and current accepted "best practices" in clinical trials.…”

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confidence: 99%

“…Literature can be found on recommendations, with some suggesting device companies work toward the optimal clinical trial design and others suggesting cultural and understanding of clinical trial design be reformed. Recommendations also include the consideration that long term data is crucial to understand the device, safety and effectiveness, and can provide insight into new considerations and uses for the device [7].…”

mentioning

confidence: 99%

“…Industry and academia expertise can be complimented by national and international regulatory guidance in consideration of best practices in clinical trial design. While clinical trials in medical devices may not be able to provide doubleblinded advantage, endpoint assessments in patient quality of life and subjective responses are valuable for the industry [7]. In ongoing evaluations, masking the investigator will allow distinct advantage in these newly considered endpoints.…”

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confidence: 99%

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Medical device transformation without delay

Babyar¹

2017

Saf Health

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The medical device industry is a significant and major contributor to global health, yet innovation and research remains suboptimal. Current data focuses on devices, recalls and economics without genuine reflection on health impact and outcomes. Additionally, current understanding of medical device innovation and regulation has provided recommendations that have yet to be implemented. The medical device industry has ample opportunity to transform. Recommendations in strengthening pre and post market data, clinical trial parameters and impact, measurement of health outcomes and global surveillance can advance this transformation. Acknowledgement of ongoing successes in reform, such as device exemption approval turnaround times, can be a catalyst for the larger industry. Health service and outcome research, improved policies and application of recommendations can transform medical devices for best practice and optimal global health.

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“…Over 43% of these studies did not use any comparator and enrolled a median number of patients of 241. The median duration of primary effectiveness end point follow-up was 3 months 8 .…”

mentioning

confidence: 99%