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A Novel Family of Toxoplasma IMC Proteins Displays a Hierarchical Organization and Functions in Coordinating Parasite Division

机译:弓形虫IMC蛋白的新型家族在协调寄生虫司显示层次结构和功能。

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摘要

Apicomplexans employ a peripheral membrane system called the inner membrane complex (IMC) for critical processes such as host cell invasion and daughter cell formation. We have identified a family of proteins that define novel sub-compartments of the Toxoplasma gondii IMC. These IMC Sub-compartment Proteins, ISP1, 2 and 3, are conserved throughout the Apicomplexa, but do not appear to be present outside the phylum. ISP1 localizes to the apical cap portion of the IMC, while ISP2 localizes to a central IMC region and ISP3 localizes to a central plus basal region of the complex. Targeting of all three ISPs is dependent upon N-terminal residues predicted for coordinated myristoylation and palmitoylation. Surprisingly, we show that disruption of ISP1 results in a dramatic relocalization of ISP2 and ISP3 to the apical cap. Although the N-terminal region of ISP1 is necessary and sufficient for apical cap targeting, exclusion of other family members requires the remaining C-terminal region of the protein. This gate-keeping function of ISP1 reveals an unprecedented mechanism of interactive and hierarchical targeting of proteins to establish these unique sub-compartments in the Toxoplasma IMC. Finally, we show that loss of ISP2 results in severe defects in daughter cell formation during endodyogeny, indicating a role for the ISP proteins in coordinating this unique process of Toxoplasma replication.
机译:蚜虫复合体采用称为内膜复合物(IMC)的外围膜系统处理关键过程,例如宿主细胞入侵和子代细胞形成。我们已经确定了定义弓形虫IMC的新小隔间的蛋白质家族。这些IMC亚室蛋白ISP1、2和3在整个Apicomplexa中都是保守的,但似乎不在门外。 ISP1定位到IMC的顶盖部分,而ISP2定位到IMC的中央区域,ISP3定位到复合体的中央加基础区域。所有三个ISP的目标都取决于预测的豆蔻酰化和棕榈酰化协同作用的N末端残基。令人惊讶的是,我们表明ISP1的破坏导致ISP2和ISP3急剧地重新定位到根尖。尽管ISP1的N末端区域对于根尖帽定位是必要且足够的,但排除其他家族成员则需要蛋白质的其余C末端区域。 ISP1的这种守门功能揭示了一种前所未有的蛋白质相互作用和分级靶向机制,可在弓形虫IMC中建立这些独特的亚区室。最后,我们表明ISP2的丢失会导致内吞发生过程中子细胞形成的严重缺陷,表明ISP蛋白在协调这种独特的弓形虫复制过程中发挥了作用。

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