The penton base of adenovirus mediates viral attachment to integrin receptors and particle internalisation, properties that can be exploited to reengineer prokariotic viruses for the infection of mammalian cells. We report that filamentous phage displaying either the full-length penton base gene or a central region of 107 amino acids on their surface were able to bind, internalise, and transduce mammalian cells expressing integrin receptors. Both phage bound avb3, avb5, a3b1, and a5b1 integrin subtypes. Cell-binding was shown by electron microscopy; internalisation was investigated by immunofluorescence and confirmed by micropanning. As it has been described for adenovirus, pharmacologic disruption of phosphoinositide-30H kinase, but not of myosin light-chain kinase, inhibited phage internalisation. Recombinant phage encoding an eukaryotic expression cassette was able to mediate gene expression in mammalian cells. Taken together, these data open insights for the exploit of recombinant phage for integrin-targeted gene delivery.
Binding properties, cell delivery, and gene transfer of adenoviral penton base displaying bacteriophage / DI GIOVINE, Monica; Salone, Barbara; Yuri, Martina; Amati, Valentina; Giovanna, Zambruno; Enrico, Cundari; Cristina M., Failla; Saggio, Isabella. - In: VIROLOGY. - ISSN 0042-6822. - STAMPA. - 282:1(2001), pp. 102-112. [10.1006/viro.2000.0809]
Binding properties, cell delivery, and gene transfer of adenoviral penton base displaying bacteriophage
DI GIOVINE, Monica;SALONE, Barbara;AMATI, VALENTINA;SAGGIO, Isabella
2001
Abstract
The penton base of adenovirus mediates viral attachment to integrin receptors and particle internalisation, properties that can be exploited to reengineer prokariotic viruses for the infection of mammalian cells. We report that filamentous phage displaying either the full-length penton base gene or a central region of 107 amino acids on their surface were able to bind, internalise, and transduce mammalian cells expressing integrin receptors. Both phage bound avb3, avb5, a3b1, and a5b1 integrin subtypes. Cell-binding was shown by electron microscopy; internalisation was investigated by immunofluorescence and confirmed by micropanning. As it has been described for adenovirus, pharmacologic disruption of phosphoinositide-30H kinase, but not of myosin light-chain kinase, inhibited phage internalisation. Recombinant phage encoding an eukaryotic expression cassette was able to mediate gene expression in mammalian cells. Taken together, these data open insights for the exploit of recombinant phage for integrin-targeted gene delivery.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
