首页> 外文期刊>Veterinary Parasitology >Peripheral blood mononuclear cell supernatants from asymptomatic dogs immunized and experimentally challenged with Leishmania chagasi can stimulate canine macrophages to reduce infection in vitro.
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Peripheral blood mononuclear cell supernatants from asymptomatic dogs immunized and experimentally challenged with Leishmania chagasi can stimulate canine macrophages to reduce infection in vitro.

机译:对无症状犬进行免疫和实验性利什曼原虫的攻击后,其外周血单核细胞上清液可以刺激犬巨噬细胞减少体外感染。

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Leishmania chagasi is the causative agent of visceral leishmaniasis in both humans and dogs in the New World. The dog is the main domestic reservoir and its infection displays different clinical presentations, from asymptomatic to severe disease. Macrophages play an important role in the control of Leishmania infection. Although it is not an area of intense study, some data suggest a role for canine macrophages in parasite killing by a NO-dependent mechanism. It has been proposed that control of human disease could be possible with the development of an effective vaccine against canine visceral leishmaniasis. Development of a rapid in vitro test to predict animal responses to Leishmania infection or vaccination should be helpful. In this study, an in vitro model was established to test whether peripheral blood mononuclear cell (PBMC) supernatants from dogs immunized with promastigote lysates and infected with L. chagasi promastigotes could stimulate macrophages from healthy dogs in order to control parasite infection. PBMC from a majority of the immunized and experimentally infected dogs expressed IFN- gamma mRNA and secreted IFN- gamma when stimulated with soluble L. chagasi antigen (SLA) in vitro. Additionally, the supernatants from stimulated PBMC were able to reduce the percentage of infected donor macrophages. The results also indicate that parasite killing in this system is dependent on NO, since aminoguanidine (AMG) reversed this effect. This in vitro test appears to be useful for screening animal responses to parasite inoculation as well as studying the lymphocyte effector mechanisms involved in pathogen killing by canine macrophages..
机译:南美白斑利什曼原虫是新世界中人和狗内脏利什曼病的病原体。狗是主要的家畜,其感染表现出从无症状到严重疾病的不同临床表现。巨噬细胞在控制利什曼原虫感染中起重要作用。尽管这不是一个深入研究的领域,但是一些数据表明,犬巨噬细胞在通过NO依赖性机制杀死寄生虫中发挥了作用。已经提出,通过开发针对犬内脏利什曼病的有效疫苗可以控制人类疾病。进行快速体外测试以预测动物对利什曼原虫感染或疫苗接种的反应将有所帮助。在这项研究中,建立了一个体外模型来测试用前鞭毛体裂解物免疫并感染了南美锥虫乳杆菌的狗的外周血单核细胞(PBMC)上清液是否可以刺激健康犬的巨噬细胞以控制寄生虫感染。在体外用可溶性恰加斯氏乳杆菌抗原(SLA)刺激后,来自大多数免疫和实验感染狗的PBMC表达IFN-γmRNA,并分泌IFN-γ。另外,来自刺激的PBMC的上清液能够减少感染的供体巨噬细胞的百分比。结果还表明,由于氨基胍(AMG)逆转了这种效应,因此该系统中的寄生虫杀伤作用依赖于NO。这项体外试验似乎可用于筛选动物对寄生虫接种的反应,以及研究与犬巨噬细胞杀死病原体有关的淋巴细胞效应器机制。

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