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Genome-wide diversity and gene expression profiling of Babesia microti isolates identify polymorphic genes that mediate host-pathogen interactions

机译:巴氏杆菌分离株的全基因组多样性和基因表达谱鉴定出介导宿主-病原体相互作用的多态性基因

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摘要

Babesia microti, a tick-transmitted, intraerythrocytic protozoan parasite circulating mainly among small mammals, is the primary cause of human babesiosis. While most cases are transmitted by Ixodes ticks, the disease may also be transmitted through blood transfusion and perinatally. A comprehensive analysis of genome composition, genetic diversity, and gene expression profiling of seven B. microti isolates revealed that genetic variation in isolates from the Northeast United States is almost exclusively associated with genes encoding the surface proteome and secretome of the parasite. Furthermore, we found that polymorphism is restricted to a small number of genes, which are highly expressed during infection. In order to identify pathogen-encoded factors involved in host-parasite interactions, we screened a proteome array comprised of 174 B. microti proteins, including several predicted members of the parasite secretome. Using this immuno-proteomic approach we identified several novel antigens that trigger strong host immune responses during the onset of infection. The genomic and immunological data presented herein provide the first insights into the determinants of B. microti interaction with its mammalian hosts and their relevance for understanding the selective pressures acting on parasite evolution.
机译:小巴贝虫(Babysia microti)是tick传播的红细胞内原生动物寄生虫,主要在小型哺乳动物中传播,是人类巴贝西虫病的主要原因。虽然大多数情况是通过I虱传播的,但该病也可能通过输血和围产期传播。对七个小肠弯曲杆菌分离株的基因组组成,遗传多样性和基因表达谱的综合分析表明,来自美国东北部分离株的遗传变异几乎完全与编码该寄生虫的表面蛋白质组和分泌组的基因有关。此外,我们发现多态性仅限于少数在感染过程中高度表达的基因。为了鉴定参与宿主-寄生虫相互作用的病原体编码因子,我们筛选了由174 B. microti蛋白组成的蛋白质组阵列,其中包括寄生虫分泌组的几个预测成员。使用这种免疫蛋白质组学方法,我们确定了几种新型抗原,它们在感染发作时触发了强烈的宿主免疫反应。本文介绍的基因组和免疫学数据提供了对小肠芽孢杆菌与其哺乳动物宿主相互作用决定因素的初步见解,以及它们与了解作用于寄生虫进化的选择性压力的相关性。

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