| Literature DB >> 26983756 |
Caterina Ieranò1, Luigi Portella1, Sara Lusa2, Giuseppina Salzano3, Crescenzo D'Alterio1, Maria Napolitano1, Maria Buoncervello4, Daniele Macchia4, Massimo Spada4, Antonio Barbieri5, Antonio Luciano5, Maria Vittoria Barone6, Lucia Gabriele4, Michele Caraglia7, Claudio Arra5, Giuseppe De Rosa2, Stefania Scala1.
Abstract
The chemokine CXCL12 activates CXCR4, initiating multiple pathways that control immune cell trafficking, angiogenesis and embryogenesis; CXCR4 is also overexpressed in multiple tumors affecting metastatic dissemination. While there has been great enthusiasm for exploiting the CXCR4-CXCL12 axis as a target in cancer therapy, to date the promise has yet to be fulfilled. A new class of CXCR4-antagonist cyclic peptides was recently developed and the compound named Peptide R was identified as the most active. With the intent to improve the efficacy and biodistribution of Peptide R, stealth liposomes decorated with Peptide R were developed (PL-Peptide R). In vitro PL-Peptide R efficiently inhibited CXCR4-dependent migration and in vivo it significantly reduced lung metastases and increased overall survival in B16-CXCR4 injected C57BL/6 mice. To evaluate if PL-Peptide R could also be a drug delivery system for CXCR4 expressing tumors, the PL-Peptide R was loaded with doxorubicin (DOX) (PL-Peptide R-DOX). PL-Peptide R-DOX efficiently delivered DOX to CXCR4 expressing cell lines with a consequent decrease in the DOX IC50 efficient dose. In vivo, B16-CXCR4 injected C57BL/6 mice treated with PL-Peptide R-DOX developed fewer lung metastases compared to PL-DOX treated mice. This work provides the proof-of-concept to prevent metastasis by using combined nanomedicine.Entities:
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Year: 2016 PMID: 26983756 DOI: 10.1039/c5nr06335c
Source DB: PubMed Journal: Nanoscale ISSN: 2040-3364 Impact factor: 7.790