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首页> 外文期刊>Scandinavian journal of immunology. >A Non‐pathogenic Recombinant Leishmania Leishmania Expressing Lipophosphoglycan 3 Against Experimental Infection with Leishmania infantum Leishmania infantum
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A Non‐pathogenic Recombinant Leishmania Leishmania Expressing Lipophosphoglycan 3 Against Experimental Infection with Leishmania infantum Leishmania infantum

机译:一种非致病重组Leishmania Leishmania,表达脂磷酸亚磷脂3与Leishmania Infantum Leishmania Infantum的实验感染

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Abstract Visceral leishmaniasis ( VL ) is caused by Leishmania infantum in the Mediterranean basin and affects primarily children and immunosuppressed individuals. Various strategies of vaccination have so far been examined by either protein or DNA without achievable complete protection against the disease. The live non‐pathogenic lizard parasite, Leishmania tarentolae , expressing elected Leishmania antigens has recently provided a promising new approach as a safe and effective live vaccine candidate to prevent leishmaniasis. Here, we evaluated the immunoprotective potential of a live recombinant L.?tarentolae expressing Lipophosphoglycan 3 ( LPG 3) antigen against L.?infantum infection in BALB /c mice. Results indicated that the administration of live recombinant Leishmania produced a significant high level of IFN ‐ γ accompanied by reduced levels of IL ‐10 as compared to wild‐type parasites as live vaccine control, thus suggesting the induction of a Th1‐type immune response in a mouse model of visceral leishmaniasis. Analysis of the IgG antibody response also showed high levels of IgG2a relative to IgG1 in sera of mice immunized with recombinant Leishmania parasites. However, immune responses elicited by this live vaccine conferred partial protection against infectious challenge. Therefore, further studies are required to increase its protective efficacy.
机译:抽象的内脏LeishManiaisis(VL)是由地中海盆地的Leishmania Infantum引起的,主要影响儿童和免疫抑制的个体。迄今为止,蛋白质或DNA检查了各种疫苗疫苗策略,而不可实现对疾病的完全保护。 The live non‐pathogenic lizard parasite, Leishmania tarentolae , expressing elected Leishmania antigens has recently provided a promising new approach as a safe and effective live vaccine candidate to prevent leishmaniasis.在这里,我们评估了在Balb / C小鼠中表达脂磷酸亚胺3(LPG 3)抗原的活重组L.Ontartolae的免疫保护潜力。结果表明,与野生型寄生虫作为活疫苗控制相比,Leishant Leishmania的施用显着高水平的IFN-γ伴随着IL-10水平降低,因此表明Th1型免疫应答的诱导鼠标模型的内脏利伊曼病。 IgG抗体反应的分析还显示出高水平的IgG2A相对于用重组Leishmania寄生虫免疫的小鼠血清中的IgG1。然而,这种活疫苗引起的免疫应答赋予了局部保护免受传染性挑战。因此,需要进一步的研究来增加其保护效率。

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