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Protection against bubonic and pneumonic plague with a single dose microencapsulated sub-unit vaccine

机译:用单剂量微囊化亚单位疫苗预防鼠疫和肺鼠疫

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Protection against virulent plague challenge by the parenteral and aerosol routes was afforded by a single administration of microencapsulated Caf1 and LcrV antigens from Yersinia pestis in BALB/c mice. Recombinant Caf1 and LcrV were individually encapsulated in polymeric microspheres, to the surface of which additional antigen was adsorbed. The microspheres containing either Caf1 or LcrV were blended and used to immunise mice on a single occasion, by either the intra-nasal or intra-muscular route. Both routes of immunisation induced systemic and local immune responses, with high levels of serum IgG being developed in response to both vaccine antigens. In Elispot assays, secretion of cytokines by spleen and draining lymph node cells was demonstrated, revealing activation of both Th1 and Th2 associated cytokines; and spleen cells from animals immunised by either route were found to proliferate in vitro in response to both vaccine antigens. Virulent challenge experiments demonstrated that non-invasive immunisation by intra-nasal instillation can provide strong systemic and local immune responses and protect against high level challenge. Microencapsulation of these vaccine antigens has the added advantage that controlled release of the antigens occurs in vivo, so that protective immunity can be induced after only a single immunising dose.
机译:通过在BALB / c小鼠中单次施用鼠疫耶尔森氏菌的微囊化Caf1和LcrV抗原,可以防止肠胃外和气溶胶途径对鼠疫的猛烈感染。重组Caf1和LcrV分别封装在聚合物微球中,其表面吸附了其他抗原。混合含有Caf1或LcrV的微球,并通过鼻内或肌肉内途径一次用于免疫小鼠。两种免疫途径均引起全身和局部免疫应答,其中对两种疫苗抗原均产生高水平的血清IgG。在Elispot分析中,证实了脾脏和引流淋巴结细胞分泌细胞因子,从而揭示了Th1和Th2相关细胞因子的激活。发现通过这两种途径免疫的动物的脾细胞和脾细胞在体外均对两种疫苗抗原有反应。毒性攻毒实验表明,通过鼻内滴注进行的非侵入性免疫可以提供强大的全身和局部免疫应答,并能抵御高水平的攻毒。这些疫苗抗原的微囊化具有附加的优势,即在体内发生抗原的受控释放,因此仅需单次免疫剂量即可诱导保护性免疫。

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