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宿主抗体对恶性疟原虫毒力抗原表达的全球选择

Global selection of Plasmodium falciparum virulence antigen expression by host antibodies.

作者信息

Abdi Abdirahman I, Warimwe George M, Muthui Michelle K, Kivisi Cheryl A, Kiragu Esther W, Fegan Gregory W, Bull Peter C

机构信息

KEMRI-Wellcome Trust Research Programme, P.O. Box 230-80108, Kilifi, Kenya.

Department of Biochemistry and Chemistry, Pwani University, P.O. Box 195, 80108, Kilifi, Kenya.

出版信息

Sci Rep. 2016 Jan 25;6:19882. doi: 10.1038/srep19882.

Abstract

Parasite proteins called PfEMP1 that are inserted on the surface of infected erythrocytes, play a key role in the severe pathology associated with infection by the Plasmodium falciparum malaria parasite. These proteins mediate binding of infected cells to the endothelial lining of blood vessels as a strategy to avoid clearance by the spleen and are major targets of naturally acquired immunity. PfEMP1 is encoded by a large multi-gene family called var. Mutually-exclusive transcriptional switching between var genes allows parasites to escape host antibodies. This study examined in detail the patterns of expression of var in a well-characterized sample of parasites from Kenyan Children. Instead of observing clear inverse relationships between the expression of broad sub-classes of PfEMP1, we found that expression of different PfEMP1 groups vary relatively independently. Parasite adaptation to host antibodies also appears to involve a general reduction in detectable var gene expression. We suggest that parasites switch both between different PfEMP1 variants and between high and low expression states. Such a strategy could provide a means of avoiding immunological detection and promoting survival under high levels of host immunity.

摘要

插入受感染红细胞表面的称为PfEMP1的寄生虫蛋白,在与恶性疟原虫感染相关的严重病理过程中起关键作用。这些蛋白介导受感染细胞与血管内皮衬里的结合,作为一种避免被脾脏清除的策略,并且是自然获得性免疫的主要靶点。PfEMP1由一个名为var的大型多基因家族编码。var基因之间相互排斥的转录转换使寄生虫能够逃避宿主抗体。本研究详细检查了来自肯尼亚儿童的特征明确的寄生虫样本中var的表达模式。我们没有观察到PfEMP1广泛亚类表达之间明显的负相关关系,而是发现不同PfEMP1组的表达相对独立地变化。寄生虫对宿主抗体的适应似乎也涉及可检测到的var基因表达普遍降低。我们认为寄生虫在不同的PfEMP1变体之间以及高表达和低表达状态之间进行转换。这样的策略可以提供一种避免免疫检测并在高水平宿主免疫下促进生存的方法。

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