| Literature DB >> 27524282 |
Giulio Fracasso1, Elisabetta Falvo2, Gianni Colotti2, Francesco Fazi3, Tiziano Ingegnere4, Adriana Amalfitano5, Giovanni Battista Doglietto6, Sergio Alfieri6, Alberto Boffi7, Veronica Morea2, Giamaica Conti8, Elisa Tremante4, Patrizio Giacomini4, Alessandro Arcovito9, Pierpaolo Ceci10.
Abstract
Human ferritin heavy chain (HFt) has been demonstrated to possess considerable potential for targeted delivery of drugs and diagnostic agents to cancer cells. Here, we report the development of a novel HFt-based genetic construct (HFt-MP-PAS) containing a short peptide linker (MP) between each HFt subunit and an outer shielding polypeptide sequence rich in proline (P), serine (S) and alanine (A) residues (PAS). The peptide linker contains a matrix-metalloproteinases (MMPs) cleavage site that permits the protective PAS shield to be removed by tumor-driven proteolytic cleavage within the tumor microenvironment. For the first time HFt-MP-PAS ability to deliver doxorubicin to cancer cells, subcellular localization, and therapeutic efficacy on a xenogeneic mouse model of a highly refractory to conventional chemotherapeutics type of cancer were evaluated. HFt-MP-PAS-DOXO performance was compared with the novel albumin-based drug delivery system INNO-206, currently in phase III clinical trials. The results of this work provide solid evidence indicating that the stimuli-sensitive, long-circulating HFt-MP-PAS nanocarriers described herein have the potential to be exploited in cancer therapy.Entities:
Keywords: Doxorubicin (PubChem CID: 31703); Drug-delivery; Ferritin; INNO-206 (PubChem CID: 9810709); Nuclear localization; PASylation; Pancreatic cancer; Protein-cage nanocarrier
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Year: 2016 PMID: 27524282 DOI: 10.1016/j.jconrel.2016.08.010
Source DB: PubMed Journal: J Control Release ISSN: 0168-3659 Impact factor: 9.776