首页> 外文期刊>Infection and immunity >Two Epitopes Shared by Taenia crassiceps andTaenia solium Confer Protection against Murine T. crassiceps Cysticercosis along with a Prominent T1 Response
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Two Epitopes Shared by Taenia crassiceps andTaenia solium Confer Protection against Murine T. crassiceps Cysticercosis along with a Prominent T1 Response

机译:Taenia crassiceps和Taenia solium共有的两个表位可保护小鼠M. crassiceps囊尾Cy病以及突出的T1反应

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Taenia crassiceps recombinant antigens KETc1 and KETc12 have been shown to induce high level of protection against experimental murine T. crassiceps cysticercosis, an experimental model successfully used to test candidate antigens for use in vaccination against porcine Taenia solium cysticercosis. Based on the deduced amino acid sequence, KETc1 and KETc12 were chemically synthesized in linear form. Immunization with KETc1 induced 66.7 to 100% protection against murine cysticercosis, and immunization with KETc12 induced 52.7 to 88.1% protection. The elicited immune response indicated that both peptides contain at least one B-cell epitope (as demonstrated by their ability to induce specific antibodies) and one T-cell epitope that strongly stimulated the proliferation of T cells primed with either the free peptide or total cysticercal T. crassiceps antigens. The high percentage of spleen cells expressing inflammatory cytokines points to the likelihood of a T1 response being involved in protection. The protective capacity of the peptides and their presence in all developmental stages of T. solium point to these two epitopes as strong candidates for inclusion in a polyepitopic synthetic vaccine against T. solium pig cysticercosis.
机译:已显示 Taenia crassiceps 重组抗原KETc1和KETc12对实验性鼠 T具有高水平的保护作用。猪ass虫囊尾rc病,一种成功用于测试候选抗原的实验模型,用于疫苗接种猪Ta虫Ta虫病。基于推导的氨基酸序列,以线性形式化学合成KETc1和KETc12。用KETc1免疫诱导对鼠类囊尾%病的保护率为66.7%至100%,而用KETc12免疫则诱导为52.7%至88.1%的保护率。引发的免疫应答表明,两种肽均包含至少一个B细胞表位(如其诱导特异性抗体的能力所证实)和一个T细胞表位,它们强烈刺激以游离肽或总囊性细胞为载体的T细胞的增殖 T。狂犬病抗原。表达炎症细胞因子的脾细胞百分比高,表明T1反应参与保护的可能性。在 T的所有发育阶段,肽的保护能力及其存在。 solium 指出这两个表位是抗 T的多表位合成疫苗中的强候选者。猪lium虫病。

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