Sage Journals: Discover world-class research

Abstract

Background:

Pivotal clinical trials provide critical evidence to regulators regarding a product’s suitability for marketing approval. The objectives of this study are (1) to characterize select features of trials for oncology products approved by the U.S. Food and Drug Administration between 2015 and 2017; and (2) to quantify the costs of these trials and how such costs varied based on trial characteristics.

Methods:

We identified novel oncology therapeutic drugs, and their respective pivotal trials, approved between 2015 and 2017 using annual summary reports from the Food and Drug Administration. Cost estimates for each pivotal trial were calculated using IQVIA’s CostPro, a clinical trial cost estimating tool based on executed contracts between pharmaceutical manufacturers and contract research organizations. Measures of drug and trial characteristics included trial design, end point, patient enrollment, and regulatory pathway. We also performed sensitivity analyses that varied assumptions regarding how efficiently each trial was conducted.

Results:

A total of 39 pivotal clinical trials provided the basis for Food and Drug Administration approval of 30 new oncology drugs from 2015 to 2017. Among these trials, primary end points were objective response rate in 20 (51.3%), progression-free survival in 13 (33.3%), and overall survival in 6 (15.4%). Twenty trials (51.3%) were single-arm studies. The median estimated cost of oncology pivotal trials was $31.7 million (interquartile range = $17.0–$60.4 million). Trials with objective response rate as primary end point had a median estimate of $17.7 million (interquartile range = $11.9–$27.1 million), compared with trials examining progression-free survival ($42.3 million, interquartile range = $34.6–$101.2 million) or overall survival ($79.4 million, interquartile range = $56.9–$97.7 million) (p < 0.001). Estimated costs for single-arm trials ($17.7 million, interquartile range = $11.9–$23.7 million) were less than for trials with a placebo-controlled ($56.7 million, interquartile range = $40.9–$103.9 million) or active control arm ($67.6 million, IQR = $35.5–$93.5 million) (p < 0.001).

Conclusions:

Relative to the estimated costs of drug development, the costs of these oncology pivotal trials were modest, with trials that produced more valuable scientific information costing more than their counterparts.

Keywords

Cost oncology clinical trial

Get full access to this article

View all access options for this article.

References

Kinch

MS.

An analysis of FDA-approved drugs for oncology. Drug Discov Today 2014; 19(12): 1831–1835.

Richey

Lyons

Nebeker

, et al. Accelerated approval of cancer drugs: improved access to therapeutic breakthroughs or early release of unsafe and ineffective drugs. J Clin Oncol 2009; 27(26): 4398–4405.

Wellman-Labadie

Zhou

The US Orphan Drug Act: rare disease research stimulator or commercial opportunity?

Health Policy 2010; 95: 216–228.

Federal Food, Drug, And Cosmetic Act (P.L. 75-717, 1938), §505(c) and (d).

Goldberg

Wei

Fernandez

The evolution of clinical trials in oncology: defining who benefits from new drugs using innovative study designs. Oncologist 2017; 22(9): 1015–1019.

Wong

Capasso

Eckhardt

SG.

The changing landscape of phase I trials in oncology. Nat Rev Clin Oncol 2016; 13: 106–117.

Hilal

Sonbol

Prasad

Analysis of control arm quality in randomized clinical trials leading to anticancer drug approval by the US Food and Drug Administration. JAMA Oncol 2019; 5(6): 887–892.

Chen

Raghunathan

Prasad

An overview of cancer drugs approved by the US Food and Drug Administration based on the surrogate end point of response rate. JAMA Intern Med 2019; 179(7): 915–921.

Dalton

Sullivan

Ecsedy

, et al. Patient enrichment for precision-based cancer clinical trials: using prospective cohort surveillance as an approach to improve clinical trials. Clin Pharmacol Ther 2018; 104(1): 23–26.

10.

Moore

Zhang

Anderson

, et al. Estimated costs of pivotal trials for novel therapeutic agents approved by the US Food and Drug Administration, 2015-2016. JAMA Intern Med 2018; 178(11): 1451–1457.

11.

Qiao

Alexander

Moore

TJ.

Globalization of clinical trials: variation in estimated regional costs of pivotal trials, 2015–2016. Clin Trials 2019; 16(3): 329–333.

12.

U.S. Food and Drug Administration Center for Drug Evaluation Research. Novel drug approvals for 2015, https://www.fda.gov/drugs/new-drugs-fda-cders-new-molecular-entities-and-new-therapeutic-biological-products/novel-drug-approvals-2015 (accessed 1 March 2019).

13.

U.S. Food and Drug Administration Center for Drug Evaluation Research. Novel drug approvals for 2016, https://www.fda.gov/drugs/new-drugs-fda-cders-new-molecular-entities-and-new-therapeutic-biological-products/novel-drug-approvals-2016 (accessed 1 March 2019).

14.

U.S. Food and Drug Administration Center for Drug Evaluation Research. Novel drug approvals for 2017, https://www.fda.gov/drugs/new-drugs-fda-cders-new-molecular-entities-and-new-therapeutic-biological-products/novel-drug-approvals-2017 (accessed 1 March 2019).

15.

IQVIA. Clinical Trial Optimization Solutions, https://www.iqvia.com/solutions/technologies/clinical-trial-design-and-planning-suite/clinical-trial-optimization-solutions (accessed 15 February 2019).

16.

Eisenstein

Lemons

2nd Tardiff

, et al. Reducing the costs of phase III cardiovascular clinical trials. Am Heart J 2005; 149(3): 482–488.

17.

Prasad

Mailankody

Research and development spending to bring a single cancer drug to market and revenues after approval. JAMA Intern Med 2017; 177(11): 1569–1575.

18.

Prasad

De Jesus

Mailankody

The high price of anticancer drugs: origins, implications, barriers, solutions. Nat Rev Clin Oncol 2017; 14(6): 381–390.

19.

IQVIA Institute for human data science. Global oncology trends 2018, https://www.iqvia.com/insights/the-iqvia-institute/reports/global-oncology-trends-2018 (accessed 5 March 2019)

20.

Kesselheim

Avorn

Sarpatwari

The high cost of prescription drugs in the United States: origins and prospects for reform. JAMA 2016; 316(8): 858–871.

21.

Kesselheim

Tan

Avorn

The roles of academia, rare diseases, and repurposing in the development of the most transformative drugs. Health Aff 2015; 34(2): 286–293.

22.

Kim

Prasad

Cancer drugs approved on the basis of a surrogate end point and subsequent overall survival: an analysis of 5 years of US Food and Drug Administration approvals. JAMA Intern Med 2015; 175: 1992–1994.

23.

Fojo

Mailankody

Unintended consequences of expensive cancer therapeutics—the pursuit of marginal indications and a me-too mentality that stifles innovation and creativity. JAMA Otolaryngol Head Neck Surg 2014; 140(12): 1225–1236.

24.

Chen

Joshi

Tran

, et al. Estimation of study time reduction using surrogate end points rather than overall survival in oncology clinical trials. JAMA Intern Med 2019; 179(5): 642–647.

25.

Gyawali

Hey

Kesselheim

AS.

Assessment of the clinical benefit of cancer drugs receiving accelerated approval. JAMA Intern Med 2019; 179(7): 906–913.

26.

Kovic

Jin

Kennedy

, et al. Evaluating progression-free survival as a surrogate outcome for health-related quality of life in oncology: a systematic review and quantitative analysis. JAMA Intern Med 2018; 178(12): 1586–1596.

Supplementary Material

Please find the following supplemental material available below.

For Open Access articles published under a Creative Commons License, all supplemental material carries the same license as the article it is associated with.

For non-Open Access articles published, all supplemental material carries a non-exclusive license, and permission requests for re-use of supplemental material or any part of supplemental material shall be sent directly to the copyright owner as specified in the copyright notice associated with the article.

0.00 MB

0.43 MB

Estimated costs of pivotal trials for U.S. Food and Drug Administration–approved cancer drugs,2015–2017

Abstract

Background:

Methods:

Results:

Conclusions:

Keywords

Get full access to this article

References

Supplementary Material