Precision oncology: A new era of cancer clinical trials - PubMed (original) (raw)

Review

Precision oncology: A new era of cancer clinical trials

Lindsay A Renfro et al. Cancer Lett. 2017.

Abstract

Traditionally, site of disease and anatomic staging have been used to define patient populations to be studied in individual cancer clinical trials. In the past decade, however, oncology has become increasingly understood on a cellular and molecular level, with many cancer subtypes being described as a function of biomarkers or tumor genetic mutations. With these changes in the science of oncology have come changes to the way we design and perform clinical trials. Increasingly common are trials tailored to detect enhanced efficacy in a patient subpopulation, e.g. patients with a known biomarker value or whose tumors harbor a specific genetic mutation. Here, we provide an overview of traditional and newer biomarker-based trial designs, and highlight lessons learned through implementation of several ongoing and recently completed trials.

Keywords: Adaptive design; Biomarker-based design; Clinical trial; Oncology.

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Conflict of interest statement

STATEMENT The authors have no conflicts of interest to disclose

Figures

Figure 1. Design Schematics

a. Enrichment or Targeted Design. R = randomization M+=marker positive, M−=marker negative TA=Targeted Agent b. Marker Stratified or Marker-by-Treatment Interaction Design. R = randomization M+=marker positive, M−=marker negative TA=Targeted Agent c. Marker Strategy Design. R = randomization. d. Modified Marker Strategy Design. R = randomization, TA = Targeted Agent. e. Umbrella Design. R = randomization. TA = Targeted Agent. SoC = Standard of Care. RCT = randomized controlled trial. f. Adaptive Design. R = randomization. TA = Targeted Agent. SoC = Standard of Care. g. Basket Trial Design. TA = Targeted Agent.

Figure 1. Design Schematics

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Precision oncology: A new era of cancer clinical trials - PubMed (original) (raw)