Nano-multilamellar lipid vesicles (NMVs) enhance protective antibody responses against Shiga toxin (Stx2a) produced by enterohemorrhagic Escherichia coli strains (EHEC)

被引:0
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作者
M. J. Rodrigues-Jesus
W. L. Fotoran
R. M. Cardoso
K. Araki
G. Wunderlich
Luís C. S. Ferreira
机构
[1] Institute of Biomedical Sciences,Vaccine Development Laboratory, Department of Microbiology
[2] University of São Paulo,Unit for Drug Development and Plasmodium Molecular Biology, Department of Parasitology
[3] Institute of Biomedical Sciences,Supramolecular Chemistry and Nanotechnology Laboratory, Department of Fundamental Chemistry
[4] University of São Paulo,undefined
[5] Institute of Chemistry,undefined
[6] University of São Paulo,undefined
来源
Brazilian Journal of Microbiology | 2019年 / 50卷
关键词
Nanoparticles; Delivery system; Multilamellar vesicles; Lipids vesicles; Shiga toxin;
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学科分类号
摘要
Microlipid vesicles (MLV) have a broad spectrum of applications for the delivery of molecules, ranging from chemical compounds to proteins, in both in vitro and in vivo conditions. In the present study, we developed a new set of nanosize multilayer lipid vesicles (NMVs) containing a unique combination of lipids. The NMVs enable the adsorption of histidine-tagged proteins at the vesicle surface and were demonstrated to be suitable for the in vivo delivery of antigens. The NMVs contained a combination of neutral (DOPC) and anionic (DPPG) lipids in the inner membrane and an external layer composed of DOPC, cholesterol, and a nickel-containing lipid (DGS-NTA [Ni]). NMVs combined with a recombinant form of the B subunit of the Shiga toxin (rStx2B) produced by certain enterohemorragic Escherichia coli (EHEC) strains enhanced the immunogenicity of the antigen after parenteral administration to mice. Mice immunized with rStx2B-loaded NMVs elicited serum antibodies capable of neutralizing the toxic activities of the native toxin; this result was demonstrated both in vitro and in vivo. Taken together, these results demonstrated that the proposed NMVs represent an alternative for the delivery of antigens, including recombinant proteins, generated in different expression systems.
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页码:67 / 77
页数:10
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