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Duchenne muscular dystrophy (DMD) is characterized by the loss of a functional dystrophin protein; the muscles of DMD patients progressively degenerate as a result of mechanical stress during contractions, and the condition eventually leads to premature death. By means antisense oligonucleotides (AONs), it is possible to modulate pre-mRNA splicing eliminating mutated exons and restoring dystrophin open reading frame. To overcome the hurdles in using AONs for therapeutic interventions, we exerted engineered human DMD stem cells with a lentivirus, which permanently and efficiently delivered the cloned AONs. Here we describe for the first time the exosome-mediated release of AONs from engineered human DMD CD133+ stem cells allowing the rescue of murine dystrophin expression. Finally, upon release, AONs could be internalized by host cells suggesting a potential role of exosomes acting as vesicular carriers for DMD gene therapy.

Stem cell-mediated exon skipping of the dystrophin gene by the bystander effect / M. Meregalli, A. Farini, C. Sitzia, C. Beley, P. Razini, L.M. Cassinelli, F. Colleoni, P. Frattini, N. Santo, E. Galbiati, D. Prosperi, A. Tavelli, M. Belicchi, L. Garcia, Y. Torrente. - In: CURRENT GENE THERAPY. - ISSN 1566-5232. - 15:6(2015 Sep 29), pp. 563-571. [10.2174/1566523215666150929111400]

Stem cell-mediated exon skipping of the dystrophin gene by the bystander effect

M. Meregalli;A. Farini;P. Razini;L.M. Cassinelli;F. Colleoni;P. Frattini;N. Santo;M. Belicchi;Y. Torrente
2015

Abstract

Duchenne muscular dystrophy (DMD) is characterized by the loss of a functional dystrophin protein; the muscles of DMD patients progressively degenerate as a result of mechanical stress during contractions, and the condition eventually leads to premature death. By means antisense oligonucleotides (AONs), it is possible to modulate pre-mRNA splicing eliminating mutated exons and restoring dystrophin open reading frame. To overcome the hurdles in using AONs for therapeutic interventions, we exerted engineered human DMD stem cells with a lentivirus, which permanently and efficiently delivered the cloned AONs. Here we describe for the first time the exosome-mediated release of AONs from engineered human DMD CD133+ stem cells allowing the rescue of murine dystrophin expression. Finally, upon release, AONs could be internalized by host cells suggesting a potential role of exosomes acting as vesicular carriers for DMD gene therapy.
English
Settore MED/26 - Neurologia
Articolo
Esperti anonimi
Pubblicazione scientifica
29-set-2015
CURRENT GENE THERAPY
Bentham Science
15
6
563
571
9
Pubblicato
Periodico con rilevanza internazionale
WOS:000364566400004
2-s2.0-84947923771
Aderisco
info:eu-repo/semantics/article
Stem cell-mediated exon skipping of the dystrophin gene by the bystander effect / M. Meregalli, A. Farini, C. Sitzia, C. Beley, P. Razini, L.M. Cassinelli, F. Colleoni, P. Frattini, N. Santo, E. Galbiati, D. Prosperi, A. Tavelli, M. Belicchi, L. Garcia, Y. Torrente. - In: CURRENT GENE THERAPY. - ISSN 1566-5232. - 15:6(2015 Sep 29), pp. 563-571. [10.2174/1566523215666150929111400]
none
Prodotti della ricerca::01 - Articolo su periodico
15
262
Article (author)
no
M. Meregalli, A. Farini, C. Sitzia, C. Beley, P. Razini, L.M. Cassinelli, F. Colleoni, P. Frattini, N. Santo, E. Galbiati, D. Prosperi, A. Tavelli, M....espandi
01 - Articolo su periodico
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/323142
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