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F-肌动蛋白和肌球蛋白 F 控制着顶体拉长的动力学,从而驱动顶体与中心体的关联。

F-actin and myosin F control apicoplast elongation dynamics which drive apicoplast-centrosome association in .

机构信息

Department of Molecular and Cell Biology, University of Connecticut , Storrs, Connecticut, USA.

出版信息

mBio. 2023 Oct 31;14(5):e0164023. doi: 10.1128/mbio.01640-23. Epub 2023 Sep 21.

Abstract

and most other parasites in the phylum Apicomplexa contain an apicoplast, a non-photosynthetic plastid organelle required for fatty acid, isoprenoid, iron-sulfur cluster, and heme synthesis. Perturbation of apicoplast function results in parasite death. Thus, parasite survival critically depends on two cellular processes: apicoplast division to ensure every daughter parasite inherits a single apicoplast, and trafficking of nuclear encoded proteins to the apicoplast. Despite the importance of these processes, there are significant knowledge gaps in regards to the molecular mechanisms which control these processes; this is particularly true for trafficking of nuclear-encoded apicoplast proteins. This study provides crucial new insight into the timing of apicoplast protein synthesis and trafficking to the apicoplast. In addition, this study demonstrates how apicoplast-centrosome association, a key step in the apicoplast division cycle, is controlled by the actomyosin cytoskeleton.

摘要

并且大多数质体生物门的其他寄生虫都含有质体,这是一种非光合质体细胞器,对于脂肪酸、异戊二烯、铁硫簇和血红素的合成是必需的。质体功能的扰乱会导致寄生虫死亡。因此,寄生虫的生存严重依赖于两个细胞过程:质体分裂以确保每个子寄生虫都继承一个质体,以及核编码蛋白向质体的运输。尽管这些过程很重要,但对于控制这些过程的分子机制仍然存在很大的知识空白;对于核编码质体蛋白的运输尤其如此。本研究为质体蛋白合成和向质体运输的时间提供了重要的新见解。此外,本研究还展示了质体-中心体的关联,这是质体分裂周期中的一个关键步骤,是如何被肌动球蛋白细胞骨架控制的。

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