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Chitosan-alginate microparticulate delivery system for an alternative route of administration of BCG vaccine

机译:壳聚糖-海藻酸盐微粒输送系统用于卡介苗疫苗的替代给药途径

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摘要

Immunisation against M. tuberculosis with current available BCG vaccine lacks efficacy in preventing adult pulmonary tuberculosis. Targeting nasal mucosa is an attractive option for a more effective immunization. The delivery of BCG via the intranasal route involves overcoming barriers such as crossing the physical barrier imposed by the mucus layer and ciliar remotion, cellular uptake and intracellular trafficking byantigen presenting cells. Due to its biodegradable, immunogenic and mucoadhesive properties, chitosan particulate deliverysystems can act both as vaccine carrier and adjuvant, improving the elicited immune response. In this study, different combinations of Chitosan/Alginate/TPP microparticles with BCG were produced as vaccine systems. The developed microparticlesystem successfully modulates BCG surface physicochemical properties and promotes effective intracellular uptake by humanmacrophage cell lines Preliminary immune responses were evaluated after s.c. and intranasal immunisation of BALB/c mice. BCG vaccination successfully stimulated the segregation of IgG2a and IgG1, where intranasal immunisation with chitosan/alginate particulate system efficiently elicited a more equilibratedcellular/humoral immune response.
机译:当前可用的卡介苗疫苗对结核分枝杆菌的免疫缺乏预防成人肺结核的功效。靶向鼻粘膜是更有效免疫的诱人选择。经由鼻内途径的BCG递送涉及克服障碍,例如越过由粘液层和纤毛运动施加的物理障碍,细胞吸收和抗原呈递细胞的细胞内运输。由于其生物可降解,免疫原性和粘膜粘附特性​​,壳聚糖微粒递送系统既可以充当疫苗载体又可以作为佐剂,从而改善引发的免疫反应。在这项研究中,壳聚糖/藻酸盐/ TPP微粒与BCG的不同组合被用作疫苗系统。发达的微粒系统成功地调节了BCG表面的理化性质并促进了人类巨噬细胞细胞系对细胞内有效摄取的能力。和BALB / c小鼠的鼻内免疫。 BCG疫苗接种成功地刺激了IgG2a和IgG1的分离,其中用壳聚糖/藻酸盐颗粒系统进行鼻内免疫有效地引发了更加平衡的细胞/体液免疫反应。

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