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丝状肌动蛋白和肌球蛋白F控制着顶质体的伸长动态,这种动态驱动了刚地弓形虫中顶质体与中心体的结合。

F-actin and Myosin F control apicoplast elongation dynamics which drive apicoplast-centrosome association in Toxoplasma gondii.

作者信息

Devarakonda Parvathi Madhavi, Sarmiento Valeria, Heaslip Aoife T

出版信息

bioRxiv. 2023 Jun 29:2023.01.01.521342. doi: 10.1101/2023.01.01.521342.

Abstract

Toxoplasma gondii contains an essential plastid organelle called the apicoplast that is necessary for fatty acid, isoprenoid, and heme synthesis. Perturbations affecting apicoplast function or inheritance lead to parasite death. The apicoplast is a single copy organelle and therefore must be divided so that each daughter parasite inherits an apicoplast during cell division. In this study we identify new roles for F-actin and an unconventional myosin motor, TgMyoF, in this process. First, loss of TgMyoF and actin lead to an accumulation of apicoplast vesicles in the cytosol indicating a role for this actomyosin system in apicoplast protein trafficking or morphological integrity of the organelle. Second, live cell imaging reveals that during division the apicoplast is highly dynamic, exhibiting branched, U-shaped and linear morphologies that are dependent on TgMyoF and actin. In parasites where movement was inhibited by the depletion of TgMyoF, the apicoplast fails to associate with the parasite centrosomes. Thus, this study provides crucial new insight into mechanisms controlling apicoplast-centrosome association, a vital step in the apicoplast division cycle, which ensures that each daughter inherits a single apicoplast.

摘要

刚地弓形虫含有一种名为顶质体的重要质体细胞器,它对脂肪酸、类异戊二烯和血红素的合成至关重要。影响顶质体功能或遗传的干扰会导致寄生虫死亡。顶质体是单拷贝细胞器,因此必须进行分裂,以便每个子代寄生虫在细胞分裂过程中继承一个顶质体。在本研究中,我们确定了F-肌动蛋白和一种非常规肌球蛋白马达TgMyoF在此过程中的新作用。首先,TgMyoF和肌动蛋白的缺失导致顶质体囊泡在细胞质中积累,表明这种肌动球蛋白系统在顶质体蛋白运输或细胞器的形态完整性中发挥作用。其次,活细胞成像显示,在分裂过程中,顶质体高度动态,呈现出依赖于TgMyoF和肌动蛋白的分支、U形和线性形态。在因TgMyoF缺失而运动受抑制的寄生虫中,顶质体无法与寄生虫中心体结合。因此,本研究为控制顶质体-中心体结合的机制提供了关键的新见解,这是顶质体分裂周期中的一个重要步骤,可确保每个子代继承一个单一的顶质体。

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