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Re-defining the Golgi complex in Plasmodium falciparum using the novel Golgi marker PfGRASP

机译:使用新型高尔基标记PfGRASP重新定义恶性疟原虫中的高尔基复合体

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摘要

Plasmodium falciparum, the causative agent of malaria, relies on a sophisticated protein secretion system for host cell invasion and transformation. Although the parasite displays a secretory pathway similar to those of all eukaryotic organisms, a classical Golgi apparatus has never been described. We identified and characterised the putative Golgi matrix protein PfGRASP, a homologue of the Golgi re-assembly stacking protein (GRASP) family. We show that PfGRASP is expressed as a 70 kDa protein throughout the asexual life cycle of the parasite. We generated PfGRASP-GFP-expressing transgenic parasites and showed that this protein is localised to a single, juxtanuclear compartment in ring-stage parasites. The PfGRASP compartment is distinct from the ER, restricted within the boundaries of the parasite and colocalises with the cis-Golgi marker ERD2. Correct subcellular localisation of this Golgi matrix protein depends on a cross-species conserved functional myristoylation motif and is insensitive to Brefeldin A. Taken together our results define the Golgi apparatus in Plasmodium and depict the morphological organisation of the organelle throughout the asexual life cycle of the parasite.
机译:疟疾的病原体恶性疟原虫依赖于复杂的蛋白质分泌系统来入侵和转化宿主细胞。尽管该寄生虫显示出与所有真核生物类似的分泌途径,但从未描述过经典的高尔基体。我们确定和表征推定的高尔基体蛋白PfGRASP,高尔基体重组堆积蛋白(GRASP)家族的同源物。我们表明,PfGRASP被表达为整个寄生虫无性生活周期中的70 kDa蛋白。我们生成了表达PfGRASP-GFP的转基因寄生虫,并表明该蛋白位于环状阶段寄生虫中的单个单核室中。 PfGRASP隔室与ER不同,限制在寄生虫的边界内,并与顺式高尔基标记ERD2共定位。此高尔基体蛋白的正确亚细胞定位取决于跨物种保守的功能性肉豆蔻酰化基序,并且对布雷菲德菌素A不敏感。我们的研究结果共同定义了疟原虫中的高尔基体,并描绘了整个无性生命周期中细胞器的形态组织。寄生虫。

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