KMID : 0923620110110030163
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Immune Network 2011 Volume.11 No. 3 p.163 ~ p.168
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Formulation and Characterization of Antigen-loaded PLGA Nanoparticles for Efficient Cross-priming of the Antigen
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Lee Young-Ran
Lee Young-Hee Im Sun-A Kim Kyung-Jae Lee Chong-Kil
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Abstract
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Background: Nanoparticles (NPs) prepared from biodegradable polymers, such as poly (D,L-lactic acid-co-glycolic acid) (PLGA), have been studied as vehicles for the delivery of antigens to phagocytes. This paper describes the preparation of antigen-loaded PLGA-NPs for efficient cross-priming.
Methods: NPs containing a similar amount of ovalbumin (OVA) but different sizes were produced using a micromixer-based W/O/W solvent evaporation procedure, and the efficiency of the NPs to induce the cross-presentation of OVA peptides were examined in dendritic cells (DCs). Cellular uptake and biodistribution studies were performed using fluorescein isothiocyanate (FITC)-loaded NPs in mice.
Results: The NPs in the range of 1.1¡1.4?m in size were the most and almost equally efficient in inducing the cross- presentation of OVA peptides via H-2Kb molecules. Cellular uptake and biodistribution studies showed that opsonization of the NPs with mouse IgG greatly increased the percentage of FITC-positive cells in the spleen and lymph nodes. The major cell type of FITC-positive cells in the spleen was macrophages, whereas that of lymph nodes was DCs.
Conclusion: These results show that IgG-opsonized PLGA-NPs with a mean size of 1.1?m would be the choice of biodegradable carriers for the targeted-delivery of protein antigens for cross-priming in vivo.
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KEYWORD
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PLGA, Nanoparticle, Opsonization, Cross-priming
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