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用水溶性壳聚糖制备和表征 DwPT 三价疫苗微胶囊及其体外和体内免疫原性。

Preparation and characterization of microencapsulated DwPT trivalent vaccine using water soluble chitosan and its in-vitro and in-vivo immunological properties.

机构信息

Biochemistry Division, Department of Chemistry, Savitribai Phule Pune University (Formerly Pune University), Pune-411 007, India.

Department of Zoology, Savitribai Phule Pune University (Formerly Pune University), Pune-411 007, India.

出版信息

Int J Biol Macromol. 2018 Feb;107(Pt B):2044-2056. doi: 10.1016/j.ijbiomac.2017.10.073. Epub 2017 Oct 13.

DOI:10.1016/j.ijbiomac.2017.10.073
PMID:29037872
Abstract

The paper explained the microencapsulation of three different antigenic materials viz. Diphtheria toxoid (DT), whole cell pertussis antigens (PT and FHA) and tetanus toxoid (TT) by coacervation method using water soluble chitosan as a polymer crosslinked by vanillin/TPP co-crosslinkers for the development of oral trivalent DwPT vaccine. Instrumental characterization of chitosan microspheres suggested specific interaction with vanillin/TPP, higher thermal stability, amorphous nature, spherical morphology with size less than 2μm along with positive charge density offering mucoadhesive properties. Furthermore, PT and FHA showed higher encapsulation up to 94% followed by TT and DT. Cumulative release rate of DT was (68.47%), TT (73.67%), PT (43%) and FHA (53%). Release kinetics interpreted using DD solver program, indicated protein release followed first order kinetics and obeyed Korsmeyer-peppas model, stating fickian diffusion relates to diffusion, erosion and controlled release rate of the encapsulated toxoids. Application of formulations on caco-2 cell line showed negligible cytotoxic effect and efficient uptake of FITC labelled microspheres. The obtained in-vivo results suggests that the final trivalent DwPT formulation were having successful elicitation of both systemic (IgG) and mucosal (sIgA) immune response in balb/c mice. Overall studies indicated that DwPT formulation could be a suitable alternative to available injectable DaPT vaccine.

摘要

本文采用凝聚法将三种不同的抗原性物质(白喉类毒素(DT)、全细胞百日咳抗原(PT 和 FHA)和破伤风类毒素(TT))包封在水溶性壳聚糖微球中,壳聚糖微球由香草醛/TPP 双交联剂交联,用于开发口服三联 DwPT 疫苗。壳聚糖微球的仪器特性表明与香草醛/TPP 具有特异性相互作用、更高的热稳定性、非晶态、粒径小于 2μm 的球形形态以及带正电荷密度,提供了黏膜粘附特性。此外,PT 和 FHA 的包封率高达 94%,其次是 TT 和 DT。DT 的累积释放率为(68.47%),TT(73.67%),PT(43%)和 FHA(53%)。使用 DD 求解器程序对释放动力学进行解释,表明蛋白质释放遵循一级动力学,符合 Korsmeyer-Peppas 模型,表明菲克扩散与扩散、侵蚀和包封毒素的控制释放速率有关。制剂在 Caco-2 细胞系上的应用表明几乎没有细胞毒性作用,并且能够有效摄取 FITC 标记的微球。体内实验结果表明,最终的三联 DwPT 制剂在 Balb/c 小鼠中成功诱导了系统(IgG)和黏膜(sIgA)免疫反应。综上所述,该 DwPT 制剂可能是现有注射用 DaPT 疫苗的一种合适替代品。

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