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经血红素预处理的红细胞在体内和体外对疟原虫入侵的易感性较低。

Red Blood Cells Preconditioned with Hemin Are Less Permissive to Plasmodium Invasion In Vivo and In Vitro.

作者信息

Gaudreault Véronique, Wirbel Jakob, Jardim Armando, Rohrbach Petra, Scorza Tatiana

机构信息

Département des Sciences Biologiques, Université du Québec à Montréal, Montréal, Québec, Canada.

Institute of parasitology, McGill University, Montréal, Québec, Canada.

出版信息

PLoS One. 2015 Oct 14;10(10):e0140805. doi: 10.1371/journal.pone.0140805. eCollection 2015.

Abstract

Malaria is a parasitic disease that causes severe hemolytic anemia in Plasmodium-infected hosts, which results in the release and accumulation of oxidized heme (hemin). Although hemin impairs the establishment of Plasmodium immunity in vitro and in vivo, mice preconditioned with hemin develop lower parasitemia when challenged with Plasmodium chabaudi adami blood stage parasites. In order to understand the mechanism accounting for this resistance as well as the impact of hemin on eryptosis and plasma levels of scavenging hemopexin, red blood cells were labeled with biotin prior to hemin treatment and P. c. adami infection. This strategy allowed discriminating hemin-treated from de novo generated red blood cells and to follow the infection within these two populations of cells. Fluorescence microscopy analysis of biotinylated-red blood cells revealed increased P. c. adami red blood cells selectivity and a decreased permissibility of hemin-conditioned red blood cells for parasite invasion. These effects were also apparent in in vitro P. falciparum cultures using hemin-preconditioned human red blood cells. Interestingly, hemin did not alter the turnover of red blood cells nor their replenishment during in vivo infection. Our results assign a function for hemin as a protective agent against high parasitemia, and suggest that the hemolytic nature of blood stage human malaria may be beneficial for the infected host.

摘要

疟疾是一种寄生虫病,可在疟原虫感染的宿主中引起严重的溶血性贫血,导致氧化血红素(高铁血红素)的释放和积累。尽管高铁血红素在体外和体内都会损害疟原虫免疫力的建立,但用高铁血红素预处理的小鼠在受到恰氏疟原虫血液阶段寄生虫攻击时,其寄生虫血症水平较低。为了了解这种抗性的机制以及高铁血红素对红细胞凋亡和血浆中清除血红素结合蛋白水平的影响,在高铁血红素处理和恰氏疟原虫感染之前,用生物素标记红细胞。这种策略可以区分经高铁血红素处理的红细胞和新生的红细胞,并跟踪这两类细胞中的感染情况。对生物素化红细胞的荧光显微镜分析显示,恰氏疟原虫对红细胞的选择性增加,而高铁血红素预处理的红细胞对寄生虫入侵的易感性降低。在使用高铁血红素预处理的人红细胞进行的体外恶性疟原虫培养中,这些效应也很明显。有趣的是,高铁血红素在体内感染期间并未改变红细胞的更新率或其补充情况。我们的结果赋予了高铁血红素作为抗高寄生虫血症保护剂的功能,并表明血液阶段人类疟疾的溶血性本质可能对受感染宿主有益。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1aef/4605744/fb971881f0ef/pone.0140805.g002.jpg

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