1. Synthesis and in vitro evaluation of cyclic NGR peptide targeted thermally sensitive liposome
- Author
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Bradford J. Wood, Ayele H. Negussie, Jenna L. Miller, Goutham Reddy, Steven K. Drake, and Matthew R. Dreher
- Subjects
chemistry.chemical_classification ,Oligopeptide ,Liposome ,Antibiotics, Antineoplastic ,Stereochemistry ,Chemistry ,Temperature ,Pharmaceutical Science ,Peptide ,CD13 Antigens ,Ligand (biochemistry) ,In vitro ,Cyclic peptide ,Article ,Doxorubicin ,Cell Line, Tumor ,Cancer cell ,Liposomes ,Humans ,Oligopeptides ,Cysteine ,Protein Binding - Abstract
The Asn-Gly-Arg (NGR) motif in both cyclic and linear form has previously been shown to specifically bind to CD13/aminopeptidase N that is selectively overexpressed in tumor vasculature and some tumor cells. However, previous versions of cyclic NGR used a liable disulfide bridge between cysteine residues that may be problematic for liposome targeting due to disulfide bond formation between adjacent peptides on the liposomal surface. In this study, we report the design, synthesis, and characterization of a novel cyclic NGR-containing peptide, cKNGRE, which does not contain a disulfide bridge. cKNGRE was synthesized in good yield and purity and attached to the fluorescent reporter Oregon Green (cKNGRE-OG) and lysolipid-containing temperature sensitive liposomes (LTSLs). The identity of cKNGRE was verified with NMR and mass spectral techniques. In vitro fluorescence microscopy evaluation of cKNGRE-OG demonstrated binding and active uptake by CD13(+) cancer cells and minimal binding to CD13(-) cancer cells. The cKNGRE-OG ligand displayed 3.6-fold greater affinity for CD13(+) cancer cells than a linear NGR-containing peptide. Affinity for CD13(+) cancer cells was similarly improved 10-fold for both the cyclic and linear NGR when presented in a multivalent fashion on the surface of an LTSL. cKNGRE-targeted LTSLs rapidly released (>75% in
- Published
- 2010
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