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弓形虫中尾锚定膜蛋白靶向亚细胞细胞器的研究

Targeting of tail-anchored membrane proteins to subcellular organelles in Toxoplasma gondii.

作者信息

Padgett Leah R, Arrizabalaga Gustavo, Sullivan William J

机构信息

Department of Pharmacology and Toxicology, Indiana University School of Medicine, Indianapolis, Indiana.

Department of Microbiology and Immunology, Indiana University School of Medicine, Indianapolis, Indiana.

出版信息

Traffic. 2017 Mar;18(3):149-158. doi: 10.1111/tra.12464. Epub 2017 Jan 17.

Abstract

Proper protein localization is essential for critical cellular processes, including vesicle-mediated transport and protein translocation. Tail-anchored (TA) proteins are integrated into organellar membranes via the C-terminus, orienting the N-terminus towards the cytosol. Localization of TA proteins occurs posttranslationally and is governed by the C-terminus, which contains the integral transmembrane domain (TMD) and targeting sequence. Targeting of TA proteins is dependent on the hydrophobicity of the TMD as well as the length and composition of flanking amino acid sequences. We previously identified an unusual homologue of elongator protein, Elp3, in the apicomplexan parasite Toxoplasma gondii as a TA protein targeting the outer mitochondrial membrane. We sought to gain further insight into TA proteins and their targeting mechanisms using this early-branching eukaryote as a model. Our bioinformatics analysis uncovered 59 predicted TA proteins in Toxoplasma, 9 of which were selected for follow-up analyses based on representative features. We identified novel TA proteins that traffic to specific organelles in Toxoplasma, including the parasite endoplasmic reticulum, mitochondrion, and Golgi apparatus. Domain swap experiments elucidated that targeting of TA proteins to these specific organelles was strongly influenced by the TMD sequence, including charge of the flanking C-terminal sequence.

摘要

正确的蛋白质定位对于关键的细胞过程至关重要,包括囊泡介导的运输和蛋白质转运。尾锚定(TA)蛋白通过C末端整合到细胞器膜中,使N末端朝向细胞质溶胶。TA蛋白的定位发生在翻译后,由C末端控制,C末端包含完整的跨膜结构域(TMD)和靶向序列。TA蛋白的靶向取决于TMD的疏水性以及侧翼氨基酸序列的长度和组成。我们之前在顶复门寄生虫刚地弓形虫中鉴定出延伸因子蛋白Elp3的一个不寻常的同源物,它是一种靶向线粒体外膜的TA蛋白。我们试图以这种早期分支的真核生物为模型,进一步深入了解TA蛋白及其靶向机制。我们的生物信息学分析在弓形虫中发现了59种预测的TA蛋白,其中9种基于代表性特征被选用于后续分析。我们鉴定出了在弓形虫中运输到特定细胞器的新型TA蛋白,包括寄生虫内质网、线粒体和高尔基体。结构域交换实验表明,TA蛋白靶向这些特定细胞器受到TMD序列的强烈影响,包括侧翼C末端序列的电荷。

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