Identification and characterization of a novel peptide ligand of Tie2 for targeting gene therapy

Abstract

Tyrosine kinase with immunoglobulin and epidermal growth factor homology domain-2 (Tie2) has been considered as a rational target for gene therapy in solid tumors. In order to identify a novel peptide ligand of Tie2 for targeted gene therapy, we screened a phage display peptide library and identified a candidate peptide ligand NSLSNASEFRAPY (designated GA5). Binding assays and Scatchard analysis revealed that GA5 could specifically bind to Tie2 with a dissociation constant of 2.1 × 10-8 M. In addition, we showed that GA5 was internalized into tumor cells highly expressing Tie2. In the biodistribution assay, 125I-GA5 was mainly accumulated in SPC-A1 xenograft tumors that express Tie2. In gene delivery studies, GA5-conjugated polyethylenimine vector could achieve greater transgene transduction than non-targeted vectors both in vitro and in vivo. Tumor growth inhibition was observed in SPC-A1 xenograft-bearing mice that received eight intratumoral injections of GA5-polyethylenimine/p53 complexes in 3 weeks. The difference in tumor volume between the experiment and control groups was significant (P< 0.05). Our results showed that GA5 is a potentially efficient targeting element for cancer gene or moleculartherapy. © 2008 Institute of Biochemistry and Cell Biology, SIBS, CAS | All Rights Reserved.