A genetically modified recombinant gH625-c-prune was prepared through conjugation of c-prune with gH625, a peptide encompassing 625-644 residues of the glycoprotein H of herpes simplex virus 1, which has been proved to possess the ability to carry cargo molecules across cell membranes. C-prune is the C-terminal domain of h-prune, overexpressed in breast, colorectal, and gastric cancers, interacting with multiple partners, and representing an ideal target for inhibition of cancer development. Its C-terminal domain results in an intrinsically disordered domain (IDD), and the peculiar properties of gH625 render it an optimal candidate to act as a carrier for this net negatively charged molecule by comparison with the positively charged TAT. A characterization of the recombinant gH625-c-prune fusion protein was conducted by biochemical, cellular biology and confocal microscopy means in comparison with TAT-c-prune. The results showed that the gH625-c-prune exhibited the ability to cross biomembranes, opening a new scenario on the use of gH625 as a novel multifunctional carrier.
gH625 is a viral derived peptide for effective delivery of intrinsically disordered proteins / Smaldone, Giovanni; Falanga, Annarita; Capasso, Domenica; Guarnieri, Daniela; Correale, Stefania; Galdiero, M; Netti, PAOLO ANTONIO; Zollo, Massimo; Galdiero, Stefania; DI GAETANO, Sonia; Pedone, EMILIA MARIA. - In: INTERNATIONAL JOURNAL OF NANOMEDICINE. - ISSN 1176-9114. - 8:(2013), pp. 2555-2565. [10.2147/IJN.S44186]
gH625 is a viral derived peptide for effective delivery of intrinsically disordered proteins.
SMALDONE, GIOVANNI;FALANGA, ANNARITA;CAPASSO, DOMENICA;GUARNIERI, DANIELA;CORREALE, STEFANIA;NETTI, PAOLO ANTONIO;ZOLLO, MASSIMO;GALDIERO, STEFANIA;DI GAETANO, SONIA;PEDONE, EMILIA MARIA
2013
Abstract
A genetically modified recombinant gH625-c-prune was prepared through conjugation of c-prune with gH625, a peptide encompassing 625-644 residues of the glycoprotein H of herpes simplex virus 1, which has been proved to possess the ability to carry cargo molecules across cell membranes. C-prune is the C-terminal domain of h-prune, overexpressed in breast, colorectal, and gastric cancers, interacting with multiple partners, and representing an ideal target for inhibition of cancer development. Its C-terminal domain results in an intrinsically disordered domain (IDD), and the peculiar properties of gH625 render it an optimal candidate to act as a carrier for this net negatively charged molecule by comparison with the positively charged TAT. A characterization of the recombinant gH625-c-prune fusion protein was conducted by biochemical, cellular biology and confocal microscopy means in comparison with TAT-c-prune. The results showed that the gH625-c-prune exhibited the ability to cross biomembranes, opening a new scenario on the use of gH625 as a novel multifunctional carrier.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
