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原发性罗得西亚巴贝斯虫感染后恢复可使小鼠获得针对罗得西亚巴贝斯虫再感染和微小巴贝斯虫攻击感染的保护性免疫。

Primary Babesia rodhaini infection followed by recovery confers protective immunity against B. rodhaini reinfection and Babesia microti challenge infection in mice.

作者信息

Wang Guanbo, Efstratiou Artemis, Adjou Moumouni Paul Franck, Liu Mingming, Jirapattharasate Charoonluk, Guo Huanping, Gao Yang, Cao Shinuo, Zhou Mo, Suzuki Hiroshi, Igarashi Ikuo, Xuan Xuenan

机构信息

National Research Center for Protozoan Diseases, Obihiro University of Agriculture and Veterinary Medicine, Inada-cho, Obihiro, Hokkaido, 080-8555, Japan.

State Key Laboratory of Veterinary Biotechnology, Harbin Veterinary Research Institute, Chinese Academy of Agricultural Sciences, 427 Maduan Street, Harbin, 150001, China.

出版信息

Exp Parasitol. 2016 Oct;169:6-12. doi: 10.1016/j.exppara.2016.07.003. Epub 2016 Jul 14.

Abstract

In the present study, we investigated the protective immunity against challenge infections with Babesia rodhaini and Babesia microti in the mice recovered from B. rodhaini infection. Six groups with 5 test mice in each group were used in this study, and were intraperitoneally immunized with alive and dead B. rodhaini. The challenge infections with B. rodhaini or B. microti were performed using different time courses. Our results showed that the mice recovered from primary B. rodhaini infection exhibited low parasitemia and no mortalities after the challenge infections, whereas mock mice which had received no primary infection showed a rapid increase of parasitemia and died within 7 days after the challenge with B. rodhaini. Mice immunized with dead B. rodhaini were not protected against either B. rodhaini or B. microti challenge infections, although high titers of antibody response were induced. These results indicate that only mice immunized with alive B. rodhaini could acquire protective immunity against B. rodhaini or B. microti challenge infection. Moreover, the test mice produced high levels of antibody response and low levels of cytokines (INF-γ, IL-4, IL-12, IL-10) against B. rodhaini or B. microti after challenge infection. Mock mice, however, showed rapid increases of these cytokines, which means disordered cytokines secretion occurred during the acute stage of challenge infection. The above results proved that mice immunized with alive B. rodhaini could acquire protective immunity against B. rodhaini and B. microti infections.

摘要

在本研究中,我们调查了从罗得西亚巴贝斯虫感染中恢复的小鼠对罗得西亚巴贝斯虫和微小巴贝斯虫攻击感染的保护性免疫。本研究使用了6组,每组5只实验小鼠,并用活的和死的罗得西亚巴贝斯虫进行腹腔免疫。使用不同的时间进程进行罗得西亚巴贝斯虫或微小巴贝斯虫的攻击感染。我们的结果表明,从原发性罗得西亚巴贝斯虫感染中恢复的小鼠在攻击感染后表现出低寄生虫血症且无死亡,而未接受原发性感染的对照小鼠在受到罗得西亚巴贝斯虫攻击后寄生虫血症迅速增加并在7天内死亡。用死的罗得西亚巴贝斯虫免疫的小鼠对罗得西亚巴贝斯虫或微小巴贝斯虫的攻击感染均无保护作用,尽管诱导了高滴度的抗体反应。这些结果表明,只有用活的罗得西亚巴贝斯虫免疫的小鼠才能获得针对罗得西亚巴贝斯虫或微小巴贝斯虫攻击感染的保护性免疫。此外,实验小鼠在攻击感染后针对罗得西亚巴贝斯虫或微小巴贝斯虫产生了高水平的抗体反应和低水平的细胞因子(INF-γ、IL-4、IL-12、IL-10)。然而,对照小鼠这些细胞因子迅速增加,这意味着在攻击感染的急性期发生了细胞因子分泌紊乱。上述结果证明,用活的罗得西亚巴贝斯虫免疫的小鼠可以获得针对罗得西亚巴贝斯虫和微小巴贝斯虫感染的保护性免疫。

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