Abstract
There is a crucial need to identify new biomarkers associated with aggressive prostate cancer (PCa) including those associated with cancer stem cells (CSCs). CD44v6, generated by alternative splicing of CD44, has been proposed as a CSC biomarker due to its correlation with aggressive PCa disease. We hypothesized that phage display selected peptides that target CD44v6 may serve as theranostic agents for aggressive PCa. Here, a 15 amino acid peptide (“PFT”) was identified by affinity selection against a peptide derived from the v6 region of CD44v6. Synthesized PFT exhibited specific binding to CD44v6 with an equilibrium dissociation constant (Kd) of 743.4 nM. PFT also bound CD44v6 highly expressed on human PCa cell lines. Further, an aggressive form of PCa cells (v6A3) was isolated and tagged by a novel CSC reporter vector. The v6A3 cells had a CSC-like phenotype including enriched CD44v6 expression, enhanced clonogenicity, resistance to chemotherapeutics, and generation of heterogeneous offspring. PFT exhibited preferential binding to v6A3 cells compared to parental cells. Immunohistofluorescence studies with human PCa tissue microarrays (TMA) indicated that PFT was highly accurate in detecting CD44v6-positive aggressive PCa cells, and staining positivity was significantly higher in late stage, metastatic and higher-grade samples. Taken together, this study provides for the first time phage display selected peptides that target CD44v6 overexpressed on PCa cells. Peptide PFT may be explored as an aid in the diagnosis and therapy of advanced PCa disease.
Highlights
prostate cancer (PCa) remains the second leading cause of cancer death for men in the United States, with an estimated 161,360 new diagnosed cases and 26,730 deaths in 2017 [1]
Eleven phage clones with the highest selection frequency and unique sequences were chosen for analysis of their ability to bind the v6 region peptide using phage enzyme linked immunosorbent assay (ELISA) (Figure 1B)
The fUSE5/15mer phage displayed peptide PFT was identified and it demonstrated binding to both recombinant- and PCa cell- associated CD44v6 once chemically synthesized as a linear peptide
Summary
PCa remains the second leading cause of cancer death for men in the United States, with an estimated 161,360 new diagnosed cases and 26,730 deaths in 2017 [1]. PCa patients with localized disease have favorable long-term survival outcomes due to advances in surgical resection, androgen deprivation therapy (ADT) and chemotherapy [2]. Patients with aggressive tumors have a poor prognosis and up to 30% of these patients suffer a relapse within 18 months after surgical resection and die from disease [3]. While initially responsive to ADT, almost all PCa patients will inevitably progress to recurrent castration-resistant prostate cancer (CRPC) and die from more aggressive secondary diseases [6, 7]. There is a crucial need to identify biomarkers associated with aggressive PCa and to develop new methods to target these tumors
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