Preparation of alginate coated chitosan microparticles for vaccine delivery

BACKGROUND: Absorption of antigens onto chitosan microparticles via electrostatic interaction is a common and relatively mild process suitable for mucosal vaccine. In order to increase the stability of antigens and prevent an immediate desorption of antigens from chitosan carriers in gastrointestina...

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Autores principales: Li, XingYi, Kong, XiangYe, Shi, Shuai, Zheng, XiuLing, Guo, Gang, Wei, YuQuan, Qian, ZhiYong
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2008
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2603011/
https://www.ncbi.nlm.nih.gov/pubmed/19019229
http://dx.doi.org/10.1186/1472-6750-8-89
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author Li, XingYi
Kong, XiangYe
Shi, Shuai
Zheng, XiuLing
Guo, Gang
Wei, YuQuan
Qian, ZhiYong
author_facet Li, XingYi
Kong, XiangYe
Shi, Shuai
Zheng, XiuLing
Guo, Gang
Wei, YuQuan
Qian, ZhiYong
author_sort Li, XingYi
collection PubMed
description BACKGROUND: Absorption of antigens onto chitosan microparticles via electrostatic interaction is a common and relatively mild process suitable for mucosal vaccine. In order to increase the stability of antigens and prevent an immediate desorption of antigens from chitosan carriers in gastrointestinal tract, coating onto BSA loaded chitosan microparticles with sodium alginate was performed by layer-by-layer technology to meet the requirement of mucosal vaccine. RESULTS: The prepared alginate coated BSA loaded chitosan microparticles had loading efficiency (LE) of 60% and loading capacity (LC) of 6% with mean diameter of about 1 μm. When the weight ratio of alginate/chitosan microparticles was greater than 2, the stable system could be obtained. The rapid charge inversion of BSA loaded chitosan microparticles (from +27 mv to -27.8 mv) was observed during the coating procedure which indicated the presence of alginate layer on the chitosan microparticles surfaces. According to the results obtained by scanning electron microscopy (SEM), the core-shell structure of BSA loaded chitosan microparticles was observed. Meanwhile, in vitro release study indicated that the initial burst release of BSA from alginate coated chitosan microparticles was lower than that observed from uncoated chitosan microparticles (40% in 8 h vs. about 84% in 0.5 h). SDS-polyacrylamide gel electrophoresis (SDS-PAGE) assay showed that alginate coating onto chitosan microparticles could effectively protect the BSA from degradation or hydrolysis in acidic condition for at least 2 h. The structural integrity of alginate modified chitosan microparticles incubated in PBS for 24 h was investigated by FTIR. CONCLUSION: The prepared alginate coated chitosan microparticles, with mean diameter of about 1 μm, was suitable for oral mucosal vaccine. Moreover, alginate coating onto the surface of chitosan microparticles could modulate the release behavior of BSA from alginate coated chitosan microparticles and could effectively protect model protein (BSA) from degradation in acidic medium in vitro for at least 2 h. In all, the prepared alginate coated chitosan microparticles might be an effective vehicle for oral administration of antigens.
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spelling pubmed-26030112008-12-16 Preparation of alginate coated chitosan microparticles for vaccine delivery Li, XingYi Kong, XiangYe Shi, Shuai Zheng, XiuLing Guo, Gang Wei, YuQuan Qian, ZhiYong BMC Biotechnol Research Article BACKGROUND: Absorption of antigens onto chitosan microparticles via electrostatic interaction is a common and relatively mild process suitable for mucosal vaccine. In order to increase the stability of antigens and prevent an immediate desorption of antigens from chitosan carriers in gastrointestinal tract, coating onto BSA loaded chitosan microparticles with sodium alginate was performed by layer-by-layer technology to meet the requirement of mucosal vaccine. RESULTS: The prepared alginate coated BSA loaded chitosan microparticles had loading efficiency (LE) of 60% and loading capacity (LC) of 6% with mean diameter of about 1 μm. When the weight ratio of alginate/chitosan microparticles was greater than 2, the stable system could be obtained. The rapid charge inversion of BSA loaded chitosan microparticles (from +27 mv to -27.8 mv) was observed during the coating procedure which indicated the presence of alginate layer on the chitosan microparticles surfaces. According to the results obtained by scanning electron microscopy (SEM), the core-shell structure of BSA loaded chitosan microparticles was observed. Meanwhile, in vitro release study indicated that the initial burst release of BSA from alginate coated chitosan microparticles was lower than that observed from uncoated chitosan microparticles (40% in 8 h vs. about 84% in 0.5 h). SDS-polyacrylamide gel electrophoresis (SDS-PAGE) assay showed that alginate coating onto chitosan microparticles could effectively protect the BSA from degradation or hydrolysis in acidic condition for at least 2 h. The structural integrity of alginate modified chitosan microparticles incubated in PBS for 24 h was investigated by FTIR. CONCLUSION: The prepared alginate coated chitosan microparticles, with mean diameter of about 1 μm, was suitable for oral mucosal vaccine. Moreover, alginate coating onto the surface of chitosan microparticles could modulate the release behavior of BSA from alginate coated chitosan microparticles and could effectively protect model protein (BSA) from degradation in acidic medium in vitro for at least 2 h. In all, the prepared alginate coated chitosan microparticles might be an effective vehicle for oral administration of antigens. BioMed Central 2008-11-19 /pmc/articles/PMC2603011/ /pubmed/19019229 http://dx.doi.org/10.1186/1472-6750-8-89 Text en Copyright © 2008 Li et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License ( (http://creativecommons.org/licenses/by/2.0) ), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Li, XingYi
Kong, XiangYe
Shi, Shuai
Zheng, XiuLing
Guo, Gang
Wei, YuQuan
Qian, ZhiYong
Preparation of alginate coated chitosan microparticles for vaccine delivery
title Preparation of alginate coated chitosan microparticles for vaccine delivery
title_full Preparation of alginate coated chitosan microparticles for vaccine delivery
title_fullStr Preparation of alginate coated chitosan microparticles for vaccine delivery
title_full_unstemmed Preparation of alginate coated chitosan microparticles for vaccine delivery
title_short Preparation of alginate coated chitosan microparticles for vaccine delivery
title_sort preparation of alginate coated chitosan microparticles for vaccine delivery
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2603011/
https://www.ncbi.nlm.nih.gov/pubmed/19019229
http://dx.doi.org/10.1186/1472-6750-8-89
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