Carbosilane Glycodendrimers for Anticancer Drug Delivery: Synthetic Route, Characterization, and Biological Effect of Glycodendrimer–Doxorubicin Complexes

The complexity of drug delivery mechanisms calls for the development of new transport system designs. Here, we report a robust synthetic procedure toward stable glycodendrimer (glyco-DDM) series bearing glucose, galactose, and oligo­(ethylene glycol)-modified galactose peripheral units. In vitro cyt...

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Veröffentlicht in:Biomacromolecules 2022-01, Vol.23 (1), p.276-290
Hauptverfasser: Müllerová, Monika, Maciel, Dina, Nunes, Nádia, Wrobel, Dominika, Stofik, Marcel, Červenková Št́astná, Lucie, Krupková, Alena, Cuřínová, Petra, Nováková, Kateřina, Božík, Matěj, Malý, Marek, Malý, Jan, Rodrigues, João, Strašák, Tomáš
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Sprache:eng
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Zusammenfassung:The complexity of drug delivery mechanisms calls for the development of new transport system designs. Here, we report a robust synthetic procedure toward stable glycodendrimer (glyco-DDM) series bearing glucose, galactose, and oligo­(ethylene glycol)-modified galactose peripheral units. In vitro cytotoxicity assays showed exceptional biocompatibility of the glyco-DDMs. To demonstrate applicability in drug delivery, the anticancer agent doxorubicin (DOX) was encapsulated in the glyco-DDM structure. The anticancer activity of the resulting glyco-DDM/DOX complexes was evaluated on the noncancerous (BJ) and cancerous (MCF-7 and A2780) cell lines, revealing their promising generation- and concentration-dependent effect. The glyco-DDM/DOX complexes show gradual and pH-dependent DOX release profiles. Fluorescence spectra elucidated the encapsulation process. Confocal fluorescence microscopy demonstrated preferential cancer cell internalization of the glyco-DDM/DOX complexes. The conclusions were supported by computer modeling. Overall, our results are consistent with the assumption that novel glyco-DDMs and their drug complexes are very promising in drug delivery and related applications.
ISSN:1525-7797
1526-4602
DOI:10.1021/acs.biomac.1c01264