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首页> 外文期刊>Veterinary Parasitology >Neospora caninum tachyzoite immunome study reveals differences among three biologically different isolates
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Neospora caninum tachyzoite immunome study reveals differences among three biologically different isolates

机译:新孢子虫速殖子免疫组化研究揭示了三种生物学不同菌株之间的差异

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Pathogenesis of bovine neosporosis is determined by different host- and parasite-dependent factors, including isolate virulence. A previous study identified that several Neospora caninum tachyzoite proteins were more abundant in virulent isolates, Nc-Liv and Nc-Spain7, compared with the low-virulent isolate Nc-Spain1H. Herein, we explored differences in the immunomes of these three isolates. Protein extracts from the Nc-Liv, Nc-Spain1H and Nc-Spain7 isolates were analysed in a 3 x 3 design by 2-DE immunoblot using sera from experimentally infected mice with these same three isolates. All isolates displayed a highly similar antigenic pattern when they were assessed using the same serum. Most of the reactive spots were located in the acidic region (pH 3-7) and grouped in 3 antigenic areas (250-70, 45-37 and 35-15 KDa). Differences found in the immunome depended on the sera used, regardless of the extract employed. In this sense, sera from Nc-Liv and Nc-Spain7 infected mice recognized the highest number of antigens, followed by Nc-Spain1H infected mice sera. In fact, 4 proteins identified by MS were not consistently detected in each isolate extract by sera from low-virulent Nc-Spain1H-infected mice: serine-threonine phosphatase 2C and superoxide dismutase (related to metabolism), gliding associated protein GAP45 (related to tachyzoites invasion), and NcGRA1 (located on dense granules). Similarly, 4 non-identified spots and another 2 spots chains located in 45-37 kDa area were not detected by this pooled sera. Variations between virulent Nc-Spain7 and Nc-Liv were limited to the absence of recognition by sera from Nc-Spain7-infected mice of GAP45 and the spot chains located in the 45-37 kDa area. These results suggest that variations in the immunome profiles rely on the immune response induced by each isolate and that these differentially recognized antigens could be investigated as putative virulence markers of neosporosis. (C) 2015 Elsevier B.V. All rights reserved.
机译:牛新孢子虫病的发病机理由不同的宿主和寄生虫依赖性因素决定,包括分离毒力。先前的研究表明,与低毒力分离株Nc-Spain1H相比,强毒分离株Nc-Liv和Nc-Spain7中的几种新孢子虫速殖子蛋白含量更高。在本文中,我们探索了这三个分离株的免疫组学差异。使用来自这两个分离株的实验感染小鼠的血清,通过2-DE免疫印迹以3 x 3设计分析了Nc-Liv,Nc-Spain1H和Nc-Spain7分离株的蛋白提取物。当使用相同的血清进行评估时,所有分离株均显示出高度相似的抗原模式。大多数反应点位于酸性区(pH 3-7),并分为3个抗原区(250-70、45-37和35-15 KDa)。免疫组中发现的差异取决于所使用的血清,与所用提取物无关。从这个意义上说,Nc-Liv和Nc-Spain7感染小鼠的血清识别的抗原数量最高,其次是Nc-Spain1H感染小鼠的血清。实际上,从低毒力的Nc-Spain1H感染小鼠的血清中,每种分离物提取物中未始终检测到MS鉴定出的4种蛋白质:丝氨酸-苏氨酸磷酸酶2C和超氧化物歧化酶(与代谢有关),滑动相关蛋白GAP45(与速殖子入侵)和NcGRA1(位于致密颗粒上)。同样,该合并血清也未检测到位于45-37 kDa区域中的4个未识别斑点和另外2个斑点链。有毒的Nc-Spain7和Nc-Liv之间的变异仅限于不存在被Nc-Spain7感染的GAP45小鼠血清和位于45-37 kDa区域的斑点链识别的血清。这些结果表明,免疫组图谱的变化取决于每种分离物诱导的免疫反应,这些差异识别的抗原可以作为新孢子虫病的假定毒力标记物进行研究。 (C)2015 Elsevier B.V.保留所有权利。

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