| Literature DB >> 30187353 |
Shirleide Santos Nunes1, Renata Salgado Fernandes1, Carolina Henriques Cavalcante1, Isabela da Costa César1, Elaine Amaral Leite1, Sávia Caldeira Araújo Lopes1, Alice Ferretti2, Domenico Rubello3, Danyelle M Townsend4, Mônica Cristina de Oliveira1, Valbert Nascimento Cardoso1, André Luís Branco de Barros5,6.
Abstract
Liposomes are lipid vesicles widely used as nanocarriers in targeted drug delivery systems for therapeutic and/or diagnostic purposes. A strategy to prolong the blood circulation time of the liposomes includes the addition of a hydrophilic polymer polyethylene glycol (PEG) moiety onto the surface of the vesicle. Several studies claim that liposome PEGylation by a single chain length or a combination of PEG with different chain lengths may alter the liposomes' pharmacokinetic properties. Therefore, the purpose of this study was to evaluate the influence of PEG on the biodistribution of pH-sensitive liposomes in a tumor-bearing animal model. Three liposomal formulations (PEGylated or not) were prepared and validated to have a similar mean diameter, monodisperse distribution, and neutral zeta potential. The pharmacokinetic properties of each liposome were evaluated in healthy animals, while the biodistribution and scintigraphic images were evaluated in tumor-bearing mice. High tumor-to-muscle ratios were not statistically different between the PEGylated and non-PEGylated liposomes. While PEGylation is a well-established strategy for increasing the blood circulation of nanostructures, in our study, the use of polymer coating did not result in a better in vivo profile. Further studies must be carried out to confirm the feasibility of the non-PEGylated pH-sensitive liposomes for tumor treatment.Entities:
Keywords: Drug delivery; Liposomes; PEGylation; Tumor targeting
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Year: 2019 PMID: 30187353 PMCID: PMC6361166 DOI: 10.1007/s13346-018-0583-8
Source DB: PubMed Journal: Drug Deliv Transl Res ISSN: 2190-393X Impact factor: 4.617