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Immunogenicity of the P-8 amastigote antigen in the experimental model of canine visceral leishmaniasis

机译:P-8鞭毛鞭毛虫抗原在犬内脏利什曼病实验模型中的免疫原性

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摘要

The P-8 proteoglycolipid complex (P-8 PGLC), an amastigote antigen of Leishmania pifanoi, has been demonstrated to induce protection in mouse models, as well as to induce Tc1/Th1-like cellular responses in American cutaneous leishmaniasis patients. Because the immunization with P-8 PGLC in the murine model does not appear to be genetically restricted, we have studied the reactivity of the P-8 PGLC in Leishmania infantum infected dogs. In this study, it is shown that PBMC from experimentally infected dogs (asymptomatic, oligosymptomatic) significantly proliferated in response to soluble leishmanial antigen (SLA) or the P-8 PGLC. Further, quantification of the gene expression induced by the stimulation with P-8 in asymptomatically infected dogs showed an up-regulation of IFN-gamma and TNF-alpha, which were three to 4-fold higher than that induced by soluble Leishmania antigen (SLA). While no measurable induction of IL-10 was observed, low levels of IL-4 mRNA were observed in response to both P-8 and SLA antigens. Thus, our studies establish that P-8 is recognized by infected canines and elicits a potentially curative/protective Th1-like immune response. The identification of Leishmania antigens that elicit appropriate immune responses across different host species (humans, canine) and disease manifestations (cutaneous or visceral) could be an advantage in generating a general vaccine for leishmaniasis.
机译:P-8蛋白糖脂复合物(P-8 PGLC)是皮氏利什曼原虫的鞭毛抗原,已被证明可在小鼠模型中诱导保护作用,并在美国皮肤利什曼病患者中诱导类似Tc1 / Th1的细胞反应。因为在鼠模型中用P-8 PGLC进行免疫似乎没有遗传上的限制,所以我们研究了P-8 PGLC在婴儿利什曼原虫感染犬中的反应性。在这项研究中,表明来自实验感染狗(无症状,无症状)的PBMC对可溶性利什曼原虫抗原(SLA)或P-8 PGLC有明显的增生作用。此外,在无症状感染的狗中,通过P-8刺激诱导的基因表达的定量显示,IFN-γ和TNF-α的上调比可溶性利什曼原虫抗原(SLA)诱导的上调3至4倍)。虽然未观察到可测量的IL-10诱导,但对P-8和SLA抗原均观察到低水平的IL-4 mRNA。因此,我们的研究确定P-8被感染的犬类识别并引发潜在的治愈性/保护性Th1样免疫应答。鉴定在不同宿主物种(人类,犬类)和疾病表现形式(皮肤或内脏)中引发适当免疫应答的利什曼原虫抗原,可能是产生利什曼原虫病通用疫苗的一个优势。

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