In this study we explored the therapeutic efficacy of mAb198.3 using two drug delivery systems (DDS) for improving the targeted treatment of CRC. The mAb198.3 was either directly bound to super-paramagnetic nanoparticles (spmNPs) or embedded into human erythrocyte-based magnetized carriers, named Erythro-MagnetoHemagglutinin Virosomes (EMHVs) to produce two different novel mAb198.3 formulations. Both DDS were endowed with magnetic properties and were anchored in the target tumor site by means of an external permanent magnet. The antibody loading efficiency of these two magnetically driven drug delivery systems and the overall therapeutic efficacy of these two formulations were assessed both in vitro and in a proof-of-concept in vivo study.
Magnetically driven drug delivery systems improving targeted immunotherapy for colon-rectal cancer
Taranta MoniaFormal Analysis
;Gherardini LisaData Curation
;Giannetti AmbraMethodology
;Tombelli SaraMethodology
;Pelosi GualtieroMethodology
;Baldini FrancescoMembro del Collaboration Group
;Cinti Caterina
Ultimo
Conceptualization
2018
Abstract
In this study we explored the therapeutic efficacy of mAb198.3 using two drug delivery systems (DDS) for improving the targeted treatment of CRC. The mAb198.3 was either directly bound to super-paramagnetic nanoparticles (spmNPs) or embedded into human erythrocyte-based magnetized carriers, named Erythro-MagnetoHemagglutinin Virosomes (EMHVs) to produce two different novel mAb198.3 formulations. Both DDS were endowed with magnetic properties and were anchored in the target tumor site by means of an external permanent magnet. The antibody loading efficiency of these two magnetically driven drug delivery systems and the overall therapeutic efficacy of these two formulations were assessed both in vitro and in a proof-of-concept in vivo study.File | Dimensione | Formato | |
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prod_391428-doc_165838.pdf
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Descrizione: Magnetically driven drug delivery systems improving targeted immunotherapy for colon-rectal cancer
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