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首页> 外文期刊>BMC Infectious Diseases >Evaluation of immuno-efficacy of a novel DNA vaccine encoding Toxoplasma gondii rhoptry protein 38 (TgROP38) against chronic toxoplasmosis in a murine model
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Evaluation of immuno-efficacy of a novel DNA vaccine encoding Toxoplasma gondii rhoptry protein 38 (TgROP38) against chronic toxoplasmosis in a murine model

机译:新型弓形虫编码蛋白38(TgROP38)的DNA疫苗在鼠模型中对慢性弓形虫病的免疫效力评估

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Background Toxoplasma gondii is an obligate intracellular parasite which can infect almost all mammalian animals, leading to toxoplasmosis. T. gondii rhoptry protein 38 (TgROP38) is an active rhoptry protein kinase which is involved in the inhibitory effect on host cell transcription by down-regulating the MAPK signaling track. Methods TgROP38 gene was amplified and inserted into eukaryotic vector pVAX I and formed the DNA vaccine pVAX-ROP38. Mice in the experimental group were intramuscularly immunized with pVAX-ROP38 and those injected with pVAX I, PBS or nothing were treated as controls. After three injections at two week intervals, all mouse groups were challenged intraperitoneally with 1000 tachyzoites of the virulent T. gondii RH strain (Type I, ToxoDB #10) and 10 cysts of the PRU strain (Type II, ToxoDB #1), respectively. Results Mice inoculated with pVAX-ROP38 vaccine had a higher level of IgG antibodies (P?P?+ and CD8+ proportions in vaccinated mice were also increased significantly compared with that in mice of the three control groups (P?P? Conclusions The present study revealed that the pVAX-ROP38 vaccine could elicit strong humoral and cell immunity response against chronic T. gondii infection in mice, resulting in the reduction of the brain cyst formation effectively, which suggests that TgROP38 is a desirable vaccine candidate against chronic T. gondii infection.
机译:背景弓形虫是专性的细胞内寄生虫,可感染几乎所有的哺乳动物,导致弓形虫病。弓形虫Rhoptry蛋白38(TgROP38)是一种活性Rhoptry蛋白激酶,它通过下调MAPK信号通路参与对宿主细胞转录的抑制作用。方法扩增TgROP38基因并插入真核载体pVAX I中,形成DNA疫苗pVAX-ROP38。用pVAX-ROP38肌内免疫实验组的小鼠,并用pVAX I,PBS或什么都不注射的小鼠作为对照。在两周的间隔内进行三次注射后,分别用1000株强毒弓形虫RH菌株速殖子(I型,ToxoDB#10)和10株PRU菌株的囊肿(II型,ToxoDB#1)腹膜内攻击所有小鼠。 。结果接种pVAX-ROP38疫苗的小鼠的IgG抗体水平较高(与正常小鼠相比,接种小鼠的P?P?+ 和CD8 + 比例也明显升高)。三个对照组(P?P?)结论本研究表明,pVAX-ROP38疫苗可引起小鼠针对慢性弓形虫感染的强烈体液和细胞免疫反应,从而有效减少脑囊肿的形成,这表明TgROP38是抗慢性刚地弓形虫感染的理想候选疫苗。

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