An Overview of Cancer Drugs Approved by the US Food and Drug Administration Based on the Surrogate End Point of Response Rate

Chen, Emerson Y.; Raghunathan, Vikram; Prasad, Vinay

doi:10.1001/jamainternmed.2019.0583

Cited by 116 publications

(100 citation statements)

References 30 publications

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“…102 Over half of "single-group" studies in a recent review of cancer drug approvals had sufficiently large sample sizes to include control groups. 103 RCTs with active comparators should be more routinely used for drug and device approval. 104 Regulators should routinely investigate the availability, validity, and completeness of outcome data in existing clinical registries to facilitate embedding active-comparator trials.…”

Section: More Routine Use Of Active Comparator Rctsmentioning

confidence: 99%

Generating comparative evidence on new drugs and devices before approval

et al. 2020

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Fewer than half of new drugs have data on their comparative benefits and harms against existing treatment options at the time of regulatory approval in Europe and the US. Even when activecomparator trials exist, they may not produce meaningful data to inform decisions in clinical practice and health policy. Recently, the uncertainty associated with the paucity of well-designed active-comparator trials has been compounded by legal and regulatory changes in Europe and the US that have created a complex mix of expedited programs aimed at facilitating faster access to new drugs. Comparative evidence generation is even sparser for medical devices. Some have argued that the current process for regulatory approval needs to generate more evidence that is useful for patients, clinicians, and payers in health care systems. We propose a set of 5 key principles relevant to the European Medicines Agency (EMA), European medical device regulatory agencies, and the US Food and Drug Administration (FDA), as well as payers, that we believe will provide the necessary incentives for pharmaceutical and device companies to generate comparative data on drugs and devices and assure timely availability of evidence that is useful for decision making. First, labeling should routinely inform patients and clinicians whether comparative data exist on new products. Second, regulators should be more selective in their use of programs that facilitate drug and device approvals on the basis of incomplete benefit and harm data. Third, regulators should encourage the conduct of randomised trials with active comparators. Fourth, regulators should use prospectively-designed network meta-analyses based on existing and future randomised trials. Fifth, payers should use their policy levers and negotiating power to incentivise the generation of comparative evidence on new and existing drugs and devices, for example, by explicitly considering proven added benefit in pricing and payment decisions.

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Section: More Routine Use Of Active Comparator Rctsmentioning

confidence: 99%

Generating comparative evidence on new drugs and devices before approval

et al. 2020

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“…Randomized controlled trials (RCTs) are the gold standard to investigate efficacy of novel drug therapies and, therefore, RCTs are pivotal for drug marketing authorization applications 1–3 . However, in the accelerated approval pathway of the US Food and Drug Administration (FDA) and in the conditional marketing approval pathway of the European Medicines Agency (EMA), new and mostly expensive anticancer drugs are increasingly approved based upon studies with surrogate end points such as progression‐free survival (PFS) or objective response rate, and a large part of these studies lack a standard‐of‐care control arm 4 . Consequently, the treatment effect in terms of overall survival (OS) is unclear at approval by the authorities.…”

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confidence: 99%

An Electronic Health Record Text Mining Tool to Collect Real‐World Drug Treatment Outcomes: A Validation Study in Patients With Metastatic Renal Cell Carcinoma

Laar

Gombert-Handoko

Guchelaar

et al. 2020

Clin Pharma and Therapeutics

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Real‐world evidence can close the inferential gap between marketing authorization studies and clinical practice. However, the current standard for real‐world data extraction from electronic health records (EHRs) for treatment evaluation is manual review (MR), which is time‐consuming and laborious. Clinical Data Collector (CDC) is a novel natural language processing and text mining software tool for both structured and unstructured EHR data and only shows relevant EHR sections improving efficiency. We investigated CDC as a real‐world data (RWD) collection method, through application of CDC queries for patient inclusion and information extraction on a cohort of patients with metastatic renal cell carcinoma (RCC) receiving systemic drug treatment. Baseline patient characteristics, disease characteristics, and treatment outcomes were extracted and these were compared with MR for validation. One hundred patients receiving 175 treatments were included using CDC, which corresponded to 99% with MR. Calculated median overall survival was 21.7 months (95% confidence interval (CI) 18.7–24.8) vs. 21.7 months (95% CI 18.6–24.8) and progression‐free survival 8.9 months (95% CI 5.4–12.4) vs. 7.6 months (95% CI 5.7–9.4) for CDC vs. MR, respectively. Highest F1‐score was found for cancer‐related variables (88.1–100), followed by comorbidities (71.5–90.4) and adverse drug events (53.3–74.5), with most diverse scores on international metastatic RCC database criteria (51.4–100). Mean data collection time was 12 minutes (CDC) vs. 86 minutes (MR). In conclusion, CDC is a promising tool for retrieving RWD from EHRs because the correct patient population can be identified as well as relevant outcome data, such as overall survival and progression‐free survival.

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“…22 Cancer drugs approved by the FDA based on the surrogate endpoint of response rate were often tested in post-marketing studies that captured other similar surrogate endpoints. 29 Among high-risk therapeutic devices approved via FDA's most stringent pathway for medical devices, implementation of post-approval studies has been challenging. 30 According to one review, only approximately 13% of initiated post-marketing studies were completed between three and five years after FDA approval.…”

Section: Regulatory Agency-driven Research In the Post-marketing Periodmentioning

confidence: 99%

Generating comparative evidence on new drugs and devices after approval

et al. 2020

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Certain limitations of evidence available on drugs and devices at the time of market approval often persist in the post-marketing period. Too often, post-marketing research landscape is fragmented. When regulatory agencies require pharmaceutical and device manufacturers to conduct studies in the post-marketing period, these studies may remain incomplete many years after approval. Even when completed, many post-marketing studies lack meaningful active comparators, have observational designs, and may not collect patient-relevant outcomes. It is crucial for regulators, in collaboration with the industry and patients, to ensure that the important questions that are unanswered at the time of drug and device approval are resolved in a timely fashion during the post-marketing phase. We propose a set of seven key guiding principles that we believe will provide the necessary incentives for pharmaceutical and device manufacturers to generate comparative data in the post-marketing period. First, regulators and pharmaceutical companies (for drugs), notified bodies and manufacturers (for devices) should develop customised evidence generation plans, ensuring that future post-approval studies address any limitations of the data available at the time of market entry that would influence the benefit-risk profiles of drugs and devices. Second, post-marketing studies should be designed hierarchically: priority should be given to efforts aimed at evaluating a product's net clinical benefit in randomised trials compared with current known effective therapy, whenever possible, to address common decisional dilemmas. Third, post-marketing studies should incorporate active comparators as appropriate. Fourth, use of non-randomised studies for the evaluation of clinical benefit in the post-marketing period should be limited to instances when the magnitude of effect is deemed to be very large or when it is possible to reasonably infer the comparative benefits or risks in settings where doing a randomised trial is not feasible. Fifth, efficiency of randomised trials should be improved by streamlining patient recruitment and data collection through innovative design elements. Sixth, governments should directly support and facilitate the production of comparative post-marketing data by investing in the development of collaborative research networks and data systems that reduce the complexity, cost, and waste of rigorous postmarketing research efforts. Seventh, financial incentives and penalties should be developed or more actively reinforced.

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An Overview of Cancer Drugs Approved by the US Food and Drug Administration Based on the Surrogate End Point of Response Rate

Cited by 116 publications

References 30 publications

Generating comparative evidence on new drugs and devices before approval

Generating comparative evidence on new drugs and devices before approval

An Electronic Health Record Text Mining Tool to Collect Real‐World Drug Treatment Outcomes: A Validation Study in Patients With Metastatic Renal Cell Carcinoma

Generating comparative evidence on new drugs and devices after approval

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