首页> 外文期刊>Infection and immunity >Intranasal immunization with SAG1 protein of Toxoplasma gondii in association with cholera toxin dramatically reduces development of cerebral cysts after oral infection.
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Intranasal immunization with SAG1 protein of Toxoplasma gondii in association with cholera toxin dramatically reduces development of cerebral cysts after oral infection.

机译:弓形虫SAG1蛋白与霍乱毒素的鼻内免疫大大减少了口腔感染后脑囊肿的发展。

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摘要

SAG1 protein of Toxoplasma gondii was evaluated as a protective antigen in mucosal immunization with cholera toxin as an adjuvant. CBA/J mice intranasally immunized with a combination of SAG1 and cholera toxin exhibited significantly fewer cysts in the brain after oral infection with the 76K strain of T. gondii than control mice. This acquired protection lasted at least 5 months. Protected mice developed high levels of serum anti-SAG1 immunoglobulin G antibodies as well as an enhanced systemic cellular response, as assessed by the proliferation of splenocytes in response to SAG1 restimulation in vitro. This cellular proliferation was associated with an increase of interleukin-2 and interleukin-5 synthesis and with barely detectable gamma interferon production. Splenic immune T cells were shown to convey modest protection to recipients against development of brain cysts following oral infection with T. gondii. Significant production of anti-SAG1 immunoglobulin A was induced in intestinal secretions of protected mice. These results indicate that intranasal immunization with SAG1 and cholera toxin can induce mucosal and systemic immune responses and affords partial and long-lasting resistance against the establishment of chronic toxoplasmosis.
机译:在霍乱毒素作为佐剂的粘膜免疫中,弓形虫的SAG1蛋白被评估为保护性抗原。经SAG1和霍乱毒素联合鼻内免疫的CBA / J小鼠经弓形虫76K菌株口服感染后,脑中的囊肿明显少于对照小鼠。获得的保护至少持续了5个月。受保护的小鼠发展出高水平的血清抗SAG1免疫球蛋白G抗体以及增强的全身细胞反应,如体外对SAG1再刺激的脾细胞增殖所评估的。这种细胞增殖与白细胞介素2和白细胞介素5合成的增加以及几乎检测不到的γ干扰素产生有关。口腔感染弓形虫后,脾脏免疫T细胞显示出适度的保护作用,使受者免受脑囊肿的发展。在受保护的小鼠的肠分泌物中诱导了抗SAG1免疫球蛋白A的大量产生。这些结果表明,鼻内用SAG1和霍乱毒素免疫可以诱导粘膜和全身免疫反应,并且对建立慢性弓形体病具有部分和长期的抵抗力。

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