National Institute of Cholera and Enteric Diseases, Indian Council of Medical Research, Kolkata 700010, India.
Department of Pharmacology, Bengal School of Technology, Hooghly 712102, West Bengal, India.
Carbohydr Polym. 2015 May 5;121:403-10. doi: 10.1016/j.carbpol.2014.12.044. Epub 2015 Jan 2.
In the present study, nanoparticles of low MW chitosan (CS) were formulated in which measles antigen was entrapped and subsequently coated with sodium alginate. The size and surface properties of the nanoparticle can be tuned with different MW of CS. In vitro release studies showed initial burst release followed by extended release, best fitted in the Makoid-Banakar model (R(2)>0.98). SDS-PAGE assay revealed that alginate coating could effectively protect antigen in acidic condition for at least 2h. Cell viability was assessed using MTT assay into HT 29 cell line. Formulations were orally administered to mice and immunological responses were evaluated using ELISA method. Obtained results showed that measles antigen-loaded CS nanoparticles induced strong immune response and significant correlation was observed between the immune response with CS MW. Protecting ability of antigen in gastric environment, sustained release kinetics, systemic and mucosal immune responses and low cytotoxicity observed for the alginate coated nanoparticles demonstrated that LMW CS could be promising platform for oral vaccine delivery.
在本研究中,制备了低分子量壳聚糖(CS)的纳米颗粒,其中包封了麻疹抗原,随后用海藻酸钠进行了涂层。纳米颗粒的大小和表面性质可以通过不同的 CS 分子量进行调节。体外释放研究表明,最初有突释,随后是持续释放,最符合 Makoid-Banakar 模型(R(2)>0.98)。SDS-PAGE 分析表明,海藻酸钠涂层可以在酸性条件下至少保护抗原 2 小时。通过 MTT 测定法评估 HT 29 细胞系中的细胞活力。将制剂口服给予小鼠,并通过 ELISA 法评估免疫反应。得到的结果表明,麻疹抗原负载的 CS 纳米颗粒诱导了强烈的免疫反应,并且观察到免疫反应与 CS 分子量之间存在显著相关性。在胃环境中对抗原的保护能力、持续释放动力学、全身和黏膜免疫反应以及低细胞毒性表明,海藻酸钠涂层纳米颗粒具有口服疫苗传递的潜力。
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