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DNA 疫苗编码弓形虫缓殖子特异性表面抗原 SAG2CDX 可保护 BALB/c 小鼠免受 II 型寄生虫感染。

DNA vaccine encoding the Toxoplasma gondii bradyzoite-specific surface antigens SAG2CDX protect BALB/c mice against type II parasite infection.

机构信息

Department of Human Parasitology, Shandong University School of Medicine, No. 44 Wenhuaxi Road, Jinan, Shandong 250012, PR China.

出版信息

Vaccine. 2013 Sep 23;31(41):4536-40. doi: 10.1016/j.vaccine.2013.07.065. Epub 2013 Aug 6.

Abstract

The surface antigens SAG2C, SAG2D, and SAG2X, which expressed specifically on bradyzoite stage of Toxoplasma gondii, have been demonstrated to be important for persistence of cyst in the brain. In this study, DNA vaccines expressing SAG2C, SAG2D, and SAG2X of T. gondii were constructed and their protective efficacy were evaluated in BALB/c mice. Mice vaccinated with pVAX1-SAG2C (pSAG2C), pVAX1-2D (pSAG2D) or pVAX1-2X (pSAG2C) showed higher levels of serum IgG antibodies and lymphocyte proliferation response compared to PBS and pVAX1 treated mice (p<0.05). The immune response was characterized by a strong Th1 response and increased cytokine production of IL-2 and IFN-γ. Vaccinated mice displayed significant protection against the challenge with the cyst of T. gondii genotype II strain of PRU (cyst-forming in mouse). A significant reduction in the brain cyst burden was detected in the mice immunized with pSAG2C (72%), pSAG2D (23%), pSAG2X (69%) alone and even more reduction rate, 77%, was achieved in the combination group compared to PBS treated mice. The results implied that immunization with DNA vaccines expressing SAG2C, SAG2D, and SAG2X, and, in particular, a combination of all three DNA plasmids, could effectively protect the mice against T. gondii chronic infection.

摘要

表面抗原 SAG2C、SAG2D 和 SAG2X 特异性表达于刚地弓形虫缓殖子期,已被证明对脑内包囊的持续存在很重要。本研究构建了表达弓形虫 SAG2C、SAG2D 和 SAG2X 的 DNA 疫苗,并在 BALB/c 小鼠中评估了其保护效力。与 PBS 和 pVAX1 处理的小鼠相比,接种 pVAX1-SAG2C (pSAG2C)、pVAX1-2D (pSAG2D) 或 pVAX1-2X (pSAG2C) 的小鼠血清 IgG 抗体和淋巴细胞增殖反应水平更高 (p<0.05)。免疫反应的特征是强烈的 Th1 反应和增加的细胞因子产生,如 IL-2 和 IFN-γ。接种疫苗的小鼠对 PRU 弓形虫 II 型株囊(在小鼠中形成囊)的攻击表现出显著的保护作用。与 PBS 处理的小鼠相比,单独免疫 pSAG2C(72%)、pSAG2D(23%)、pSAG2X(69%)的小鼠脑中囊的负担显著减少,而联合组的减少率甚至更高,达到 77%。结果表明,用表达 SAG2C、SAG2D 和 SAG2X 的 DNA 疫苗免疫,特别是三种 DNA 质粒的联合免疫,可有效保护小鼠免受弓形虫慢性感染。

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