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Lipid-peptide bioconjugation through pyridyl disulfide reaction chemistry and its application in cell targeting and drug delivery

Author(s)
de la Fuente-Herreruela, DiegoMonnappa, Ajay K.Munoz-Ubeda, MonicaMorallon-Pina, AaronEnciso, EduardoSanchez, LuisGiusti, FabriceNatale, PaoloLopez-Montero, Ivan
Issued Date
2019-06
DOI
10.1186/s12951-019-0509-8
URI
https://scholarworks.unist.ac.kr/handle/201301/27251
Fulltext
https://jnanobiotechnology.biomedcentral.com/articles/10.1186/s12951-019-0509-8
Citation
JOURNAL OF NANOBIOTECHNOLOGY, v.17, no.1, pp.77
Abstract
BackgroundThe design of efficient drug delivery vectors requires versatile formulations able to simultaneously direct a multitude of molecular targets and to bypass the endosomal recycling pathway of cells. Liposomal-based vectors need the decoration of the lipid surface with specific peptides to fulfill the functional requirements. The unspecific binding of peptides to the lipid surface is often accompanied with uncontrolled formulations and thus preventing the molecular mechanisms of a successful therapy.ResultsWe present a simple synthesis pathway to anchor cysteine-terminal peptides to thiol-reactive lipids for adequate and quantitative liposomal formulations. As a proof of concept, we have synthesized two different lipopeptides based on (a) the truncated Fibroblast Growth Factor (tbFGF) for cell targeting and (b) the pH sensitive and fusogenic GALA peptide for endosomal scape.ConclusionsThe incorporation of these two lipopeptides in the liposomal formulation improves the fibroblast cell targeting and promotes the direct delivery of cargo molecules to the cytoplasm of the cell.
Publisher
BMC
ISSN
1477-3155
Keyword (Author)
Smart liposomesDisulfide bondsTargeting peptideGALAEndosomal escape
Keyword
FIBROBLAST-GROWTH-FACTORSENSITIVE FUSOGENIC PEPTIDETHIN-LAYER-CHROMATOGRAPHYFLUOROMETRIC ASSAYGENE DELIVERYALAMAR BLUELIPOSOMESNANOPARTICLESTRANSFECTIONLIPOPLEXES

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