伯氏疟原虫
毒力
生物
疟疾
寄生虫寄主
恶性疟原虫
啮齿动物
疟原虫(生命周期)
病毒学
遗传学
免疫学
基因
生态学
计算机科学
万维网
作者
Mariana De Niz,Ann-Katrin Ullrich,Arlett Heiber,Alexandra Blancke Soares,Christian Pick,Ruth Lyck,Derya Keller,Gesine Kaiser,Mónica Prado,Sven Flemming,Hernando A. del Portillo,Chris J. Janse,Volker T. Heussler,Tobias Spielmann
摘要
Sequestration of red blood cells infected with the human malaria parasite Plasmodium falciparum in organs such as the brain is considered important for pathogenicity. A similar phenomenon has been observed in mouse models of malaria, using the rodent parasite Plasmodium berghei, but it is unclear whether the P. falciparum proteins known to be involved in this process are conserved in the rodent parasite. Here we identify the P. berghei orthologues of two such key factors of P. falciparum, SBP1 and MAHRP1. Red blood cells infected with P. berghei parasites lacking SBP1 or MAHRP1a fail to bind the endothelial receptor CD36 and show reduced sequestration and virulence in mice. Complementation of the mutant P. berghei parasites with the respective P. falciparum SBP1 and MAHRP1 orthologues restores sequestration and virulence. These findings reveal evolutionary conservation of the machinery underlying sequestration of divergent malaria parasites and support the notion that the P. berghei rodent model is an adequate tool for research on malaria virulence.
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