Does biomarker use in oncology improve clinical trial failure risk? A large‐scale analysis

Jayson L. Parker; Sebnem S. Kuzulugil; Kirill Pereverzev; Stephen Mac; Gilberto Lopes; Zain Shah; Ashini Weerasinghe; Daniel Rubinger; Adam Falconi; Ayse Bener; Bora Caglayan; Rohan Tangri; Nicholas Mitsakakis

doi:10.1002/cam4.3732

Cancer Medicine (Mar 2021)

Does biomarker use in oncology improve clinical trial failure risk? A large‐scale analysis

Jayson L. Parker,
Sebnem S. Kuzulugil,
Kirill Pereverzev,
Stephen Mac,
Gilberto Lopes,
Zain Shah,
Ashini Weerasinghe,
Daniel Rubinger,
Adam Falconi,
Ayse Bener,
Bora Caglayan,
Rohan Tangri,
Nicholas Mitsakakis

Affiliations

Jayson L. Parker: Department of Biology University of Toronto Mississauga Mississauga ON Canada
Sebnem S. Kuzulugil: St Michael's Hospital Toronto ON Canada
Kirill Pereverzev: Department of Biology University of Toronto Mississauga Mississauga ON Canada
Stephen Mac: Institute of Health Policy, Management and EvaluationUniversity of Toronto Mississauga ON Canada
Gilberto Lopes: University of MiamiMiller School of Medicine Coral Gables FL USA
Zain Shah: Department of Biology University of Toronto Mississauga Mississauga ON Canada
Ashini Weerasinghe: Prevention and Cancer ControlCancer Care Ontario Toronto ON Canada
Daniel Rubinger: Department of Biology University of Toronto Mississauga Mississauga ON Canada
Adam Falconi: Department of Pharmacy Leslie Dan Faculty of Pharmacy University of Toronto Toronto ON Canada
Ayse Bener: Mechanical and Industrial Engineering Ryerson University Toronto ON Canada
Bora Caglayan: Mechanical and Industrial Engineering Ryerson University Toronto ON Canada
Rohan Tangri: Department of Biology University of Toronto Mississauga Mississauga ON Canada
Nicholas Mitsakakis: Institute of Health Policy, Management and Evaluation, and Division of BiostatisticsDalla Lana School of Public HealthUniversity of Toronto Toronto ON Canada

DOI: https://doi.org/10.1002/cam4.3732
Journal volume & issue: Vol. 10, no. 6
pp. 1955 – 1963

Abstract

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Abstract Purpose To date there has not been an extensive analysis of the outcomes of biomarker use in oncology. Methods Data were pooled across four indications in oncology drawing upon trial outcomes from www.clinicaltrials.gov: breast cancer, non‐small cell lung cancer (NSCLC), melanoma and colorectal cancer from 1998 to 2017. We compared the likelihood drugs would progress through the stages of clinical trial testing to approval based on biomarker status. This was done with multi‐state Markov models, tools that describe the stochastic process in which subjects move among a finite number of states. Results Over 10000 trials were screened, which yielded 745 drugs. The inclusion of biomarker status as a covariate significantly improved the fit of the Markov model in describing the drug trajectories through clinical trial testing stages. Hazard ratios based on the Markov models revealed the likelihood of drug approval with biomarkers having nearly a fivefold increase for all indications combined. A 12, 8 and 7‐fold hazard ratio was observed for breast cancer, melanoma and NSCLC, respectively. Markov models with exploratory biomarkers outperformed Markov models with no biomarkers. Conclusion This is the first systematic statistical evidence that biomarkers clearly increase clinical trial success rates in three different indications in oncology. Also, exploratory biomarkers, long before they are properly validated, appear to improve success rates in oncology. This supports early and aggressive adoption of biomarkers in oncology clinical trials.

Published in Cancer Medicine

ISSN: 2045-7634 (Online)
Publisher: Wiley
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Neoplasms. Tumors. Oncology. Including cancer and carcinogens
Website: https://onlinelibrary.wiley.com/journal/20457634

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