Abstract
Aim: We reviewed the radiographic response of three patients with metastatic castration-resistant prostate cancer treated with CRXL301, a docetaxel nanoparticle. For these three patients, we isolated and analyzed circulating tumor cells (CTCs) to explore microtubule (MT) drug-target engagement (MT-DTE) as a biomarker of response to treatment. MT-DTE was based on a quantitative assessment of the MT cytoskeleton in CTCs from pre- and post-treatment patient samples as a potential read-out of CRXL301 activity.Methods: We isolated CTCs using negative CD45+ depletion and subjected them to multiplex confocal microscopy using our established protocol. CTCs were identified as CD45-/CK+/DAPI+ cells and MT-DTE was determined using our developed imaging algorithm. We quantified MT bundling in CTCs across multiple time points, from baseline to on-treatment to disease progression. Here, we describe the longitudinal analysis of MT-DTE in CTCs from patients treated with CRXL301 and its correlation with response to treatment.Results: We collected CTCs at seven time points from three metastatic castration-resistant prostate cancer patients. Clinical response was evaluated by Response Evaluation Criteria in Solid Tumors (RECIST) v.1.1 criteria in those patients with measurable disease. Of the three patients enrolled, one experienced partial response (-50%) to CRXL301 and two patients were unevaluable given bone only disease. Notably, however, these two patients showed stable disease clinically based on bone scans. MT-DTE across all time points revealed that, early time points within four and 24 h of drug administration exhibited the highest levels of drug engagement (MT-DTE) as compared to baseline. However, these early time points did not correlate with clinical response. We observed that the CTCs collected one week after the first or second dose of CRXL301 treatment in the responding patient had numerically higher levels of MT-DTE as compared to the other two patients.Conclusion: Taxane on-target activity can be detected and analyzed quantitatively in CTCs by tubulin immunofluorescence. Early time points, within 24 h of drug administration, showed high levels of DTE but did not correlate with clinical response. MT-DTE in CTCs collected after one week on treatment correlated best with treatment response. The clinical utility of the 1-week CTC DTE should be tested and validated in future clinical trials involving taxanes.
Highlights
Microtubule-targeting drugs represent one of the most clinically active chemotherapy drugs for the treatment of solid tumors[1]
Clinical response was evaluated by Response Evaluation Criteria in Solid Tumors (RECIST) v.1.1 criteria in those patients with measurable disease
MT-DTE in circulating tumor cells (CTCs) collected after one week on treatment correlated best with treatment response
Summary
Microtubule-targeting drugs represent one of the most clinically active chemotherapy drugs for the treatment of solid tumors[1]. For prostate cancer, taxanes (docetaxel and cabazitaxel) are the only chemotherapy shown to prolong survival in metastatic castration-resistant prostate cancer (mCRPC) patients, and are considered standard of treatment[2,3,4,5]. Despite their clinical success, not all patients benefit from taxane treatment, while the molecular basis for taxane resistance in CRPC remains unknown. Following taxane binding to their primary cellular target, tubulin, MT stabilization and increase in MT polymer mass occur. This is indicative of effective (drug-target engagement, DTE). No clinical studies assessing MT-DTE on tumor samples have been reported yet, and the role of MT-DTE as biomarker of clinical response to taxane chemotherapy is still unclear
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