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Modulatory effects of tuberculosis vaccines on experimental autoimmune encephalomyelitis

机译:肺结核疫苗对实验性自身免疫性脑脊髓炎的调节作用

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摘要

Although BCG is the only accepted vaccine against tuberculosis (TB), its protective ability is very limited. Therefore, many new vaccines are being evaluated. Our group has been working on DNAhsp65 - a genetic construction containing the hsp65 gene from Mycobacterium leprae. In previous experimental works, we demonstrated that both DNAhsp65 alone or associated with BCG, in a prime-boost regimen, were effective to control TB. A possible deleterious effect related to autoimmunity needed to be tested because hsp65 is highly homologous to the correspondent mammalian protein. In this investigation we tested the effect of a previous immunization with DNAhsp65 alone or associated with BCG in a rat model of multiple sclerosis. Female Lewis rats were immunized with three doses of DNAhsp65 or primed with BCG followed by two DNAhsp65 boosters. The animals were, then, immunized with myelin associated with complete Freund's adjuvant to develop experimental autoimmune encephalomyelitis (EAE). The following parameters were evaluated: weight loss, clinical score, central nervous system (CNS) inflammation and anti-myelin immune response. No deleterious effect was associated with these immunizations schedules. Immunized animals equally lost weight, the clinical scores were similar and CNS inflammation did not increase. Interestingly, both procedures determined decreased inflammation in the brain and lumbar spinal cord. This was concurrent with a modulatory effect over cytokine production by peripheral lymphoid organs. Cell cultures from spleen and lymph nodes in vitro stimulated with myelin produced less IFN-gamma and IL-10, respectively. This phenomenon was more clear in rats immunized with the genetic vaccine alone than with the prime-boost strategy. Together the results suggest that these strategies for TB prophylaxis would not accelerate or aggravate multiple sclerosis, being therefore, safe in this aspect. In addition, they indicate that these vaccination regimens have a potential anti-inflammatory activity that could be better explored in the future.
机译:尽管卡介苗是唯一被接受的抗结核疫苗(TB),但其保护能力非常有限。因此,正在评估许多新疫苗。我们的小组一直在研究DNAhsp65-一种包含来自麻风分枝杆菌hsp65基因的基因构建。在先前的实验工作中,我们证明了在初免-加强疗法中,单独使用DNAhsp65或与BCG结合均可有效控制结核。由于hsp65与相应的哺乳动物蛋白高度同源,因此需要测试与自身免疫有关的可能有害作用。在这项研究中,我们在多发性硬化的大鼠模型中测试了先前单独使用DNAhsp65或与BCG联合免疫的效果。用三剂DNAhsp65免疫雌性Lewis大鼠,或先用BCG免疫,再用两种DNAhsp65加强免疫。然后,用与完全弗氏佐剂相关的髓磷脂免疫动物,以发展实验性自身免疫性脑脊髓炎(EAE)。评价以下参数:体重减轻,临床评分,中枢神经系统(CNS)炎症和抗髓磷脂免疫反应。这些免疫方案没有有害作用。免疫的动物平均体重减轻,临床评分相似,中枢神经系统炎症没有增加。有趣的是,这两种方法均确定了大脑和腰脊髓炎症的减轻。这与外周淋巴器官对细胞因子产生的调节作用同时发生。髓鞘刺激的脾脏和淋巴结体外培养的细胞分别产生较少的IFN-γ和IL-10。这种现象在仅用基因疫苗免疫的大鼠中比用初免-加强策略更清楚。在一起的结果表明,这些结核病预防策略不会加速或加重多发性硬化症,因此在这方面是安全的。此外,它们表明这些疫苗接种方案具有潜在的抗炎活性,将来可能会更好地进行探索。

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