| Literature DB >> 28941284 |
Anne-Chloé Dhez1,2,3, Elisabetta Benedetti1, Andrea Antonosante1, Gloria Panella1, Brigida Ranieri1, Tiziana M Florio1, Loredana Cristiano1, Francesco Angelucci1, Francesco Giansanti1, Luana Di Leandro1, Michele d'Angelo1, Marina Melone4,5, Antonella De Cola6, Luca Federici6, Renato Galzio1, Ilaria Cascone2,3, Fabio Raineri2,3, Annamaria Cimini1,4,7, José Courty2,3, Antonio Giordano4,8, Rodolfo Ippoliti1.
Abstract
Targeted anticancer therapies demand discovery of new cellular targets to be exploited for the delivery of toxic molecules and drugs. In this perspective, in the last few years, nucleolin has been identified as an interesting surface marker to be used for the therapy of glioblastoma. In this study, we investigated whether a synthetic antagonist of cell-surface nucleolin known as N6L, previously reported to decrease both tumor growth and tumor angiogenesis in several cancer cell lines, including glioblastoma cells, as well as endothelial cells proliferation, could be exploited to deliver a protein toxin (saporin) to glioblastoma cells. The pseudopeptide N6L cross-linked to saporin-S6 induced internalization of the toxin inside glioblastoma cancer cells. Our results in vitro demonstrated the effectiveness of this conjugate in inducing cell death, with an ID50 four orders of magnitude lower than that observed for free N6L. Furthermore, the preliminary in vivo study demonstrated efficiency in reducing the tumor mass in an orthotopic mouse model of glioblastoma.Entities:
Keywords: NucAnt (N6L); glioblastoma; nucleolin; saporin; targeted therapy
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Year: 2017 PMID: 28941284 DOI: 10.1002/jcp.26205
Source DB: PubMed Journal: J Cell Physiol ISSN: 0021-9541 Impact factor: 6.384