| Literature DB >> 30692673 |
Shan Guan1, Antje Munder2,3, Silke Hedtfeld2, Peter Braubach3,4, Silke Glage5, Longgui Zhang1, Stefan Lienenklaus5, Anja Schultze1, Günther Hasenpusch6, Wiebke Garrels5, Frauke Stanke2,3, Csaba Miskey7, Sarah M Johler1, Yadhu Kumar8, Burkhard Tümmler2,3, Carsten Rudolph1,6, Zoltan Ivics7, Joseph Rosenecker9.
Abstract
Developing safe and efficient non-viral delivery systems remains a major challenge for in vivo applications of gene therapy, especially in cystic fibrosis. Unlike conventional cationic polymers or lipids, the emerging poloxamine-based copolymers display promising in vivo gene delivery capabilities. However, poloxamines are invalid for in vitro applications and their in vivo transfection efficiency is still low compared with viral vectors. Here, we show that peptides developed by modular design approaches can spontaneously form compact and monodisperse nanoparticles with poloxamines and nucleic acids via self-assembly. Both messenger RNA and plasmid DNA expression mediated by peptide-poloxamine nanoparticles are greatly boosted in vitro and in the lungs of cystic fibrosis mice with negligible toxicity. Peptide-poloxamine nanoparticles containing integrating vectors enable successful in vitro and in vivo long-term restoration of cystic fibrosis transmembrane conductance regulator deficiency with a safe integration profile. Our dataset provides a new framework for designing non-viral gene delivery systems qualified for in vivo genetic modifications.Entities:
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Year: 2019 PMID: 30692673 DOI: 10.1038/s41565-018-0358-x
Source DB: PubMed Journal: Nat Nanotechnol ISSN: 1748-3387 Impact factor: 39.213