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BCG and BCG/DNAhsp65 Vaccinations Promote Protective Effects without Deleterious Consequences for Experimental Autoimmune Encephalomyelitis

机译:卡介苗和卡介苗/ DNAhsp65疫苗接种可促进实验性自身免疫性脑脊髓炎的保护作用而无有害后果

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摘要

A prime-boost strategy conserving BCG is considered the most promising vaccine to control tuberculosis. A boost with a DNA vaccine containing the mycobacterial gene of a heat shock protein (pVAXhsp65) after BCG priming protected mice against experimental tuberculosis. However, anti-hsp65 immunity could worsen an autoimmune disease due to molecular mimicry. In this investigation, we evaluated the effect of a previous BCG or BCG/pVAXhsp65 immunization on experimental autoimmune encephalomyelitis (EAE) development. Female Lewis rats were immunized with BCG or BCG followed by pVAXhsp65 boosters. The animals underwent EAE induction and were daily evaluated for weight loss and clinical score. They were euthanized during recovery phase to assess immune response and inflammatory infiltration at the central nervous system. Previous immunization did not aggravate or accelerate clinical score or weight loss. In addition, this procedure clearly decreased inflammation in the brain. BCG immunization modulated the host immune response by triggering a significant reduction in IL-10 and IFN-γ levels induced by myelin basic protein. These data indicated that vaccination protocols with BCG or BCG followed by boosters with pVAXhsp65 did not trigger a deleterious effect on EAE evolution.
机译:保存BCG的初免-加强策略被认为是控制结核病最有希望的疫苗。卡介苗启动后,含有热休克蛋白分枝杆菌基因(pVAXhsp65)的DNA疫苗的加强免疫保护小鼠免受实验性结核病的侵害。但是,由于分子模拟,抗hsp65免疫可能会使自身免疫性疾病恶化。在这项调查中,我们评估了以前的BCG或BCG / pVAXhsp65免疫对实验性自身免疫性脑脊髓炎(EAE)发展的影响。用BCG或BCG,然后用pVAXhsp65增强剂免疫雌性Lewis大鼠。对动物进行EAE诱导,并每天评估其体重减轻和临床评分。在恢复阶段对他们进行安乐死以评估中枢神经系统的免疫反应和炎症浸润。先前的免疫接种并未加重或加速临床评分或体重减轻。另外,该程序明显减少了脑部的炎症。 BCG免疫通过引发髓鞘碱性蛋白诱导的IL-10和IFN-γ水平的显着降低来调节宿主的免疫反应。这些数据表明,用BCG或BCG接种疫苗,然后用pVAXhsp65加强疫苗接种不会对EAE进化产生有害影响。

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