Design,Synthesis and Bioevaluation of an EphA2 Receptor‐Based Targeted Delivery System |
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| Authors: | Dr Swadesh K Das Dr Roberta Noberini Dr Russell Dahl Dr John L Stebbins Prof Elena B Pasquale Prof Paul B Fisher Prof Maurizio Pellecchia |
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| Affiliation: | 1. Department of Human & Molecular Genetics, Institute of Molecular Medicine, Massey Cancer Center, Virginia Commonwealth University School of Medicine, Sanger Hall Building, Room 11‐015, 1101 East Marshall Street, Richmond, VA 23298‐0033 (USA);2. Cancer Research Center, Sanford‐Burnham Medical Research Institute, 10901 N. Torrey Pines Rd., La Jolla, CA 92037 (USA);3. Rosalind Franklin University of Medicine & Science, College of Pharmacy, Chicago Medical School, Building: IPEC, Room: 2.80, 3333 Green Bay Road, North Chicago, Il 60064‐3095 (USA) |
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| Abstract: | Because of its overexpression in a range of solid tumors, the EphA2 receptor is a validated target for cancer therapeutics. We recently described a new targeted delivery system based on specific EphA2‐targeting peptides conjugated with the chemotherapeutic agent paclitaxel. Here, we investigate the chemical determinants responsible for the stability and degradation of these agents in plasma. Introducing modifications in both the peptide and the linker between the peptide and paclitaxel resulted in drug conjugates that are both long‐lived in rat plasma and that markedly decrease tumor size in a prostate cancer xenograft model compared with paclitaxel alone treatment. These studies identify critical rate‐limiting degradation sites on the peptide–drug conjugates, enabling the design of agents with increased stability and efficacy. These results provide support for our central hypothesis that peptide–drug conjugates targeting EphA2 represent an innovative and potentially effective strategy to selectively deliver cytotoxic drugs to cancer cells. |
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| Keywords: | chemotherapy drug discovery EphA2 ephrins targeted delivery |
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