Fougère Aurélie, Jackson Andrew P, Bechtsi Dafni Paraskevi, Braks Joanna A M, Annoura Takeshi, Fonager Jannik, Spaccapelo Roberta, Ramesar Jai, Chevalley-Maurel Séverine, Klop Onny, van der Laan Annelies M A, Tanke Hans J, Kocken Clemens H M, Pasini Erica M, Khan Shahid M, Böhme Ulrike, van Ooij Christiaan, Otto Thomas D, Janse Chris J, Franke-Fayard Blandine
Leiden Malaria Research Group, Parasitology, Center of infectious Diseases, Leiden University Medical Center (LUMC), Leiden, The Netherlands.
Department of Experimental Medicine, University of Perugia, Italy.
PLoS Pathog. 2016 Nov 16;12(11):e1005917. doi: 10.1371/journal.ppat.1005917. eCollection 2016 Nov.
Many variant proteins encoded by Plasmodium-specific multigene families are exported into red blood cells (RBC). P. falciparum-specific variant proteins encoded by the var, stevor and rifin multigene families are exported onto the surface of infected red blood cells (iRBC) and mediate interactions between iRBC and host cells resulting in tissue sequestration and rosetting. However, the precise function of most other Plasmodium multigene families encoding exported proteins is unknown. To understand the role of RBC-exported proteins of rodent malaria parasites (RMP) we analysed the expression and cellular location by fluorescent-tagging of members of the pir, fam-a and fam-b multigene families. Furthermore, we performed phylogenetic analyses of the fam-a and fam-b multigene families, which indicate that both families have a history of functional differentiation unique to RMP. We demonstrate for all three families that expression of family members in iRBC is not mutually exclusive. Most tagged proteins were transported into the iRBC cytoplasm but not onto the iRBC plasma membrane, indicating that they are unlikely to play a direct role in iRBC-host cell interactions. Unexpectedly, most family members are also expressed during the liver stage, where they are transported into the parasitophorous vacuole. This suggests that these protein families promote parasite development in both the liver and blood, either by supporting parasite development within hepatocytes and erythrocytes and/or by manipulating the host immune response. Indeed, in the case of Fam-A, which have a steroidogenic acute regulatory-related lipid transfer (START) domain, we found that several family members can transfer phosphatidylcholine in vitro. These observations indicate that these proteins may transport (host) phosphatidylcholine for membrane synthesis. This is the first demonstration of a biological function of any exported variant protein family of rodent malaria parasites.
疟原虫特异性多基因家族编码的许多变异蛋白被输出到红细胞(RBC)中。由var、stevor和rifin多基因家族编码的恶性疟原虫特异性变异蛋白被输出到受感染红细胞(iRBC)的表面,并介导iRBC与宿主细胞之间的相互作用,导致组织滞留和玫瑰花结形成。然而,编码输出蛋白的大多数其他疟原虫多基因家族的确切功能尚不清楚。为了了解啮齿动物疟原虫(RMP)红细胞输出蛋白的作用,我们通过对pir、fam-a和fam-b多基因家族成员进行荧光标记来分析其表达和细胞定位。此外,我们对fam-a和fam-b多基因家族进行了系统发育分析,结果表明这两个家族都有RMP特有的功能分化历史。我们证明,对于所有这三个家族,iRBC中家族成员的表达并非相互排斥。大多数标记蛋白被转运到iRBC细胞质中,但没有转运到iRBC质膜上,这表明它们不太可能在iRBC与宿主细胞的相互作用中发挥直接作用。出乎意料的是,大多数家族成员在肝期也有表达,在肝期它们被转运到寄生泡中。这表明这些蛋白家族通过支持肝细胞和红细胞内的寄生虫发育和/或通过操纵宿主免疫反应,促进寄生虫在肝脏和血液中的发育。事实上,对于具有类固醇生成急性调节相关脂质转运(START)结构域的Fam-A,我们发现几个家族成员在体外可以转运磷脂酰胆碱。这些观察结果表明,这些蛋白可能转运(宿主)磷脂酰胆碱用于膜合成。这是首次证明啮齿动物疟原虫任何输出变异蛋白家族的生物学功能。
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