Analytical Validation and Capabilities of the Epic CTC Platform: Enrichment-Free Circulating Tumour Cell Detection and Characterization

Shannon L. Werner; Ryon P. Graf; Mark Landers; David T. Valenta; Matthew Schroeder; Stephanie B. Greene; Natalee Bales; Ryan Dittamore; Dena Marrinucci

doi:10.33393/jcb.2015.2053

Analytical Validation and Capabilities of the Epic CTC Platform: Enrichment-Free Circulating Tumour Cell Detection and Characterization

Authors

Shannon L. Werner Epic Sciences, Inc., San Diego, CA, USA
Ryon P. Graf Epic Sciences, Inc., San Diego, CA, USA
Mark Landers Epic Sciences, Inc., San Diego, CA, USA
David T. Valenta Epic Sciences, Inc., San Diego, CA, USA
Matthew Schroeder Epic Sciences, Inc., San Diego, CA, USA
Stephanie B. Greene Epic Sciences, Inc., San Diego, CA, USA
Natalee Bales Epic Sciences, Inc., San Diego, CA, USA
Ryan Dittamore Epic Sciences, Inc., San Diego, CA, USA
Dena Marrinucci Epic Sciences, Inc., San Diego, CA, USA

DOI:

https://doi.org/10.33393/jcb.2015.2053

Keywords:

Analytical Validation, Biomarker, Circulating Tumour Cells, CTC, CTM, Clinical Feasibility, Epic CTC Platform, Fluid Biopsy, Liquid Biopsy, Metastasis

Abstract

The Epic Platform was developed for the unbiased detection and molecular characterization of circulating tumour cells (CTCs). Here, we report assay performance data, including accuracy, linearity, specificity and intra/inter-assay precision of CTC enumeration in healthy donor (HD) blood samples spiked with varying concentrations of cancer cell line controls (CLCs). Additionally, we demonstrate clinical feasibility for CTC detection in a small cohort of metastatic castrate-resistant prostate cancer (mCRPC) patients. The Epic Platform demonstrated accuracy, linearity and sensitivity for the enumeration of all CLC concentrations tested. Furthermore, we established the precision between multiple operators and slide staining batches and assay specificity showing zero CTCs detected in 18 healthy donor samples. In a clinical feasibility study, at least one traditional CTC/mL (CK+, CD45-, and intact nuclei) was detected in 89 % of 44 mCRPC samples, whereas 100 % of samples had CTCs enumerated if additional CTC subpopulations (CK-/CD45- and CK+ apoptotic CTCs) were included in the analysis. In addition to presenting Epic Platform's performance with respect to CTC enumeration, we provide examples of its integrated downstream capabilities, including protein biomarker expression and downstream genomic analyses at single cell resolution.

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Published

2015-05-05

How to Cite

Werner, S. L., Graf, R. P., Landers, M., Valenta, D. T., Schroeder, M., Greene, S. B., Bales, N., Dittamore, R., & Marrinucci, D. (2015). Analytical Validation and Capabilities of the Epic CTC Platform: Enrichment-Free Circulating Tumour Cell Detection and Characterization. Journal of Circulating Biomarkers, 4(1). https://doi.org/10.33393/jcb.2015.2053

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Issue

Vol. 4 No. 1 (2015): January-December 2015

Section

Original research article

License

Authors contributing to Journal of Circulating Biomarkers agree to publish their articles under the Creative Common Attribution Non Commercial 4.0 (CC-BY-NC 4.0) license, which allows third parties to re-use the work without permission as long as the work is properly referenced and the use is non-commercial.