Circulating Tumor Cells as a Predictor of Treatment Response in Clinically Localized Prostate Cancer

Simpa S Salami; Udit Singhal; Daniel E Spratt; Ganesh S Palapattu; Brent K Hollenbeck; Joseph D Schonhoft; Ryon Graf; Jessica Louw; Adam Jendrisak; Lyndsey Dugan; Yipeng Wang; Scott A Tomlins; Ryan Dittamore; Felix Y Feng; Todd M Morgan

doi:10.1200/po.18.00352

Circulating Tumor Cells as a Predictor of Treatment Response in Clinically Localized Prostate Cancer

JCO Precis Oncol. 2019:3:PO.18.00352. doi: 10.1200/po.18.00352. Epub 2019 May 30.

Authors

Simpa S Salami^{1

2}, Udit Singhal¹, Daniel E Spratt^{1

2}, Ganesh S Palapattu^{1

2

3}, Brent K Hollenbeck^{1

2}, Joseph D Schonhoft⁴, Ryon Graf⁴, Jessica Louw⁴, Adam Jendrisak⁴, Lyndsey Dugan⁴, Yipeng Wang⁴, Scott A Tomlins^{1

2}, Ryan Dittamore⁴, Felix Y Feng^{1

5}, Todd M Morgan^{1

2}

Affiliations

¹ Michigan Medicine, Ann Arbor, MI.
² University of Michigan Rogel Cancer Center, Ann Arbor, MI.
³ Medical University of Vienna, Vienna, Austria.
⁴ Epic Sciences, San Diego, CA.
⁵ University of San Francisco, San Francisco, CA.

Abstract

Purpose: Using nonenrichment-based, potentially more sensitive Epic Sciences circulating tumor cell (CTC) platform, we sought to detect and characterize CTCs in untreated, high-risk localized prostate cancer and to evaluate their clinical implication.

Methods: Between 2012 and 2015, blood samples were prospectively collected from patients with National Comprehensive Cancer Network high-risk localized prostate cancer undergoing either radiotherapy (XRT) plus androgen deprivation therapy or radical prostatectomy (RP) with curative intent. Samples were analyzed with the Epic Sciences platform with 4^J,6-diamidino-2-phenylindole, CD45, cytokeratin (CK), and androgen receptor (AR) N-terminal staining. CTC counts were correlated with biochemical recurrence (BCR).

Results: A diversity of CTC subtypes, including CK-positive, CK-negative, AR-positive, and CTC clusters, were observed in 73.3% (33 of 45) of patients with evaluable data. The median follow-up was 14.2 months (range, 0.5 to 43.7 months). BCR occurred more frequently in the RP group than XRT (15 of 26 v one of 19), with most patients in the XRT group continuing to receive androgen deprivation therapy. A higher proportion of metastatic events were observed in the RP group (five of 26 v one of 19). In the RP group, BCR and development of metastases were associated with a higher total number of CTCs, AR-positive CTCs, and CTC phenotypic heterogeneity. One patient who developed BCR and metastases quickly after RP had diverse phenotypical CTC subtypes, and single-cell genomic analyses of all detectable CTCs confirmed common prostate cancer copy number alterations and PTEN loss.

Conclusion: CTCs can be identified in most patients with high-risk localized prostate cancer before definitive therapy using the Epic Sciences platform. If confirmed in a larger cohort with longer follow-up, phenotypic and genomic characterization of CTCs pretherapy may provide an additional means of risk stratifying patients with newly diagnosed high-risk disease and potentially help identify patients who could require multimodal therapy.

Grants and funding

P50 CA186786/CA/NCI NIH HHS/United States