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The Lasso Segment Is Required for Functional Dimerization of the Plasmodium Formin 1 FH2 Domain

机译:套索段是疟原虫福明1 FH2域的功能二聚所需的。

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摘要

Apicomplexan parasites, such as the malaria-causing Plasmodium species, utilize a unique way of locomotion and host cell invasion. This substrate-dependent gliding motility requires rapid cycling of actin between the monomeric state and very short, unbranched filaments. Despite the crucial role of actin polymerization for the survival of the malaria parasite, the majority of Plasmodium cellular actin is present in the monomeric form. Plasmodium lacks most of the canonical actin nucleators, and formins are essentially the only candidates for this function in all Apicomplexa. The malaria parasite has two formins, containing conserved formin homology (FH) 2 and rudimentary FH1 domains. Here, we show that Plasmodium falciparum formin 1 associates with and nucleates both mammalian and Plasmodium actin filaments. Although Plasmodium profilin alone sequesters actin monomers, thus inhibiting polymerization, its monomer-sequestering activity does not compete with the nucleating activity of formin 1 at an equimolar profilin-actin ratio. We have determined solution structures of P. falciparum formin 1 FH2 domain both in the presence and absence of the lasso segment and the FH1 domain, and show that the lasso is required for the assembly of functional dimers.
机译:蚜虫寄生虫,例如引起疟疾的疟原虫种类,利用独特的运动和宿主细胞入侵的方式。这种依赖于底物的滑动运动需要肌动蛋白在单体状态和非常短的无支丝之间快速循环。尽管肌动蛋白聚合对于疟原虫的存活具有至关重要的作用,但大多数疟原虫细胞肌动蛋白仍以单体形式存在。疟原虫缺乏大多数典型的肌动蛋白成核剂,而福尔马汀本质上是所有蜂巢复合体中该功能的唯一候选者。疟疾寄生虫有两个福美宁,包含保守的formin同源性(FH)2和基本FH1结构域。在这里,我们显示恶性疟原虫福明1与哺乳动物和疟原虫肌动蛋白丝相关联并成核。尽管单独的疟原虫纤溶蛋白螯合肌动蛋白单体,从而抑制了聚合反应,但是其等价的纤溶蛋白-肌动蛋白比例下,其单体的螯合活性无法与甲酰胺1的成核活性竞争。我们已经确定了在存在和不存在套索片段和FH1域的情况下,恶性疟原虫formin 1 FH2域的溶液结构,并表明套索是功能性二聚体组装所必需的。

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